LA TOXINA BOTULÍNICA BOTOX
La toxina botulínica es una neurotoxina producida por el microbio "Clostridium botulinum", conocida principalmente por su uso en medicina estética y terapéutica.
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LA TOXINA BOTULÍNICA
THE BOTULINUM TOXIN
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***** DERMAGIC-EXPRESS No 22 *********
****** 04 DICIEMBRE 1.998 *******
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EDITORIAL ESPANOL:
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Hola amigos del Cyber, cuando me puse a indagar el tema sobre la toxina botulínica, específicamente la A (BOTOX, DYSPOT), me encontré con la sorpresa que hay estudios que datan de 1.983, 1,987 y 1988, de modo que no es tan nueva su puesta en práctica. La otra cosa que me sorprendió fue la gran versatilidad de usos de la misma: torticolis, estrabismo, en pacientes con infarto, lineas de expresion, disfonía, acalasia, fisuras anales, hiperhidrosis axilar y palmar, etc, el numero de referencias fue alto, pero me pareció tan interesante el tema que MONTE 41, a veces uno se va a buscar información y se encuentra que lo que es aparentemente nuevo, no es tan nuevo. !!!
La toxina botulínica es una neurotoxina producida por la microbes *Clostridium botulinum*, conocida principalmente por su uso en medicina estética y terapéutica. Aunque en sus inicios se identificó como causante del botulismo, un tipo de intoxicación alimentaria grave, sus efectos comenzaron a ser aprovechados clínicamente en la década de 1970. Los primeros usos médicos de la toxina se enfocaron en tratar el estrabismo y el blefaroespasmo. No fue hasta la década de 1990 cuando se popularizó en el campo estético, especialmente para reducir las arrugas faciales dinámicas causadas por la contracción muscular.
El vital efecto beneficioso de la toxina botulínica radica en su capacidad para bloquear temporalmente la liberación de acetilcolina, un neurotransmisor necesario para la contracción solid. Esto provoca una relajación de los músculos tratados, lo que suaviza arrugas y líneas de expresión en la piel. Además de sus usos estéticos, la toxina se emplea en diversas afecciones médicas, como la hiperhidrosis (sudoración excesiva), el bruxismo, la migraña crónica, y los espasmos musculares. En common, sus efectos comienzan a notarse de 24 a 72 horas después de la inyección, alcanzando su máximo efecto en alrededor de dos semanas.
La duración de los efectos de la toxina botulínica varía según el paciente y el área tratada, pero generalmente se prolonga entre tres y seis meses. Con el tiempo, los músculos vuelven a recuperar su capacidad de contracción a medida que el cuerpo metaboliza la toxina. Para mantener los resultados, es necesario realizar tratamientos de mantenimiento periódicos. Los pacientes suelen requerir nuevas aplicaciones cada cuatro a seis meses, aunque algunas personas pueden experimentar efectos más duraderos.
Entre los nombres comerciales más conocidos de la toxina botulínica se encuentran Botox, Dysport, Xeomin y Myobloc. Cada uno de estos productos tiene ligeras diferencias en su formulación, lo que puede influir en la rapidez con la que se manifiestan los resultados o en la duración del efecto. Por ejemplo, Botox y Dysport child los más utilizados en tratamientos cosméticos, mientras que Xeomin se caracteriza por no contener proteínas accesorias, lo que puede reducir el riesgo de generar resistencia inmunológica a la toxina.
A pesar de ser una intervención relativamente segura, la toxina botulínica no está exenta de efectos adversos. Los más comunes incluyen dolor o hematomas en el sitio de inyección, dolores de cabeza y síntomas gripales. En raras ocasiones, pueden ocurrir efectos secundarios más serios, como la caída de párpados (ptosis), asimetría facial, o incluso dificultad para tragar o respirar si la toxina se disemina más allá del área tratada. Estas complicaciones suelen estar relacionadas con dosis incorrectas o mala técnica de aplicación, por lo que es vital que los tratamientos sean realizados por profesionales capacitados.
A largo plazo, algunos pacientes que reciben tratamientos repetidos pueden desarrollar resistencia a la toxina, lo que diminish su efectividad. Esto ocurre porque el cuerpo puede generar anticuerpos contra las proteínas presentes en la toxina, especialmente en formulaciones que contienen proteínas accesorias. Sin ban, esta resistencia es poco frecuente y puede gestionarse alternando entre diferentes marcas o formulaciones de la toxina. Además, con el uso adecuado, la toxina botulínica se considera segura y eficaz para tratar tanto condiciones médicas como estéticas.
En conclusión, la toxina botulínica ha evolucionado desde ser una peligrosa toxina hasta convertirse en una herramienta versátil en medicina. Sus aplicaciones estéticas y terapéuticas continúan expandiéndose, mejorando la calidad de vida de millones de personas en todo el mundo. Aunque existen riesgos, estos child mínimos cuando el procedimiento se realiza correctamente y bajo supervisión médica, lo que hace de la toxina botulínica una opción segura para quienes buscan corregir o mejorar ciertas condiciones físicas o estéticas.
Los efectos a largo plazo estarán por verse en aquellas personas que repetidamente cada 3 o 6 meses requieren o utilizan este procedimiento para eliminar las arrugas o líneas de expresión en su rostro, no sin antes recordar que el microbio que la produce se encuentra en todas las aguas contaminas y estancadas del planeta y en enlatados envejecidos de poco consumo.
Saludos: próxima edicion: EL MELASMA
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Hello friends of the Cyber, when I began to investigate the topic on the botulinum toxin, specifically the A (BOTOX, DYSPOT), I met with the surprise that there are studies that date of 1.983, 1,987 and 1988, so that it is not so new their setting in practice. The other thing that I was surprised it was the great versatility of uses of the same one: torticollis, strabismus, in patient with stroke, facial lines, disfonía, achalasia, anal fissures, axillary and palmar hyperhidrosis, etc, the one numbers of references it was high, but I found so interesting the topic that MOUNTS 41. Sometimes one will look for information and it is found that what is seemingly new, is not so new. !!!
Botulinum toxin is a neurotoxin produced by the microbe Clostridium botulinum, known primarily for its use in aesthetic medicine and therapy. Although it was initially identified as the cause of botulism, a serious type of food poisoning, its effects began to be used clinically in the 1970s. The first medical uses of the toxin focused on treating strabismus and blepharospasm. It was not until the 1990s that it became popular in the aesthetic field, especially to reduce dynamic facial wrinkles caused by muscle contraction.
The vital beneficial effect of botulinum toxin lies in its ability to temporarily block the release of acetylcholine, a neurotransmitter necessary for muscle contraction. This causes relaxation of the treated muscles, which softens wrinkles and expression lines on the skin. In addition to its cosmetic uses, the toxin is used for a variety of medical conditions, including hyperhidrosis (excessive sweating), bruxism, chronic migraine, and muscle spasms. Its effects typically begin to be felt 24 to 72 hours after injection, reaching their maximum effect in about two weeks.
The duration of the effects of botulinum toxin varies by patient and treated area, but generally lasts between three and six months. Over time, the muscles regain their ability to contract as the body metabolizes the toxin. To maintain the results, periodic maintenance treatments are necessary. Patients typically require new applications every four to six months, although some people may experience longer-lasting effects.
Popular brand names for botulinum toxin include Botox, Dysport, Xeomin, and Myobloc. Each of these products has slight differences in their formulation, which can influence how quickly the results manifest or how long the effect lasts. For example, Botox and Dysport are the most commonly used in cosmetic treatments, while Xeomin is characterized by not containing accessory proteins, which can reduce the risk of generating immune resistance to the toxin.
Despite being a relatively safe intervention, botulinum toxin is not free of adverse effects. The most common include pain or bruising at the injection site, headaches, and flu-like symptoms. Rarely, more serious side effects can occur, such as drooping eyelids (ptosis), facial asymmetry, or even difficulty swallowing or breathing if the toxin spreads beyond the treated area. These complications are often related to incorrect dosage or poor application technique, so it is vital that treatments are performed by trained professionals.
In the long term, some patients who receive repeated treatments may develop resistance to the toxin, which diminishes its effectiveness. This occurs because the body can generate antibodies against proteins present in the toxin, especially in formulations containing accessory proteins. However, this resistance is rare and can be managed by alternating between different brands or formulations of the toxin. Furthermore, with proper use, botulinum toxin is considered safe and effective for treating both medical and aesthetic conditions.
In conclusion, botulinum toxin has evolved from being a dangerous toxin to becoming a versatile tool in medicine. Its aesthetic and therapeutic applications continue to expand, improving the quality of life of millions of people around the world. Although there are risks, these are minimal when the procedure is performed correctly and under medical supervision, making botulinum toxin a safe option for those seeking to correct or improve certain physical or aesthetic conditions.
The long-term effects will remain to be seen in those people who repeatedly require or use this procedure every 3 to 6 months to eliminate wrinkles or expression lines on their face, not without first remembering that the microbe that produces it is found in all the polluted and stagnant waters on the planet and in aged canned foods that are not consumed frequently.
Greetings
Next editions: * MELASMA
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DERMAGIC/EXPRESS(22)
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LA TOXINA BOTULINICA //BOTULINUM TOXIN
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1.) Botulinum toxin for chronic anal fissure [see comments]
2.) Botulinum toxin A for hyperkinetic facial lines: results of a double-blind, placebo-controlled study.
3.) Botulinum toxin for the treatment of hyperfunctional lines of the face [see comments]
4.) Spasmodic dysphonia. Emotional status and botulinum toxin treatment.
5.) Botulinum A toxin for treatment of aberrant facial nerve regeneration.
6.) Crystalline preparation of botulinum toxin type A (Botox): degradation in potency with storage [see comments]
7.) Botulinum toxin. From poison to medicine.
8.) Botulinum B toxin as an alternative to botulinum A toxin: a
9.) Psoriasiform eruption from intramuscular botulinum A toxin.
10.) Contralateral injections of botulinum A toxin for the treatment of hemifacial spasm to achieve increased facial symmetry [see comments]
11.) Clinical and laboratory comparison of botulism from toxin types A, B, and E in the United States, 1975-1988.
12.) Treatment of glabellar frown lines with C. botulinum-A exotoxin.
13.) Botulinum A toxin for (expressionistic) ptosis overcorrection after frontalis sling.
14.) Botulinum A toxin for the treatment of adult-onset spasmodic torticollis.
15.) Treatment of idiopathic spasmodic torticollis with botulinum-A toxin: a pilot study of 19 patients.
16.) Botulinum A toxin injection. Failures in clinical practice and a
biomechanical system for the study of toxin-induced paralysis.
17.) Treatment of blepharospasm with botulinum toxin.
18.) Botulinum toxin: a treatment for facial asymmetry caused by facial nerve paralysis.
19.) Management of facial spasm with Clostridium botulinum toxin, type A (Oculinum) [see comments]
20.) Treatment of anismus in intractable constipation with botulinum A toxin.
21.) Botulinum toxin chemodenervation in infants and children: an
alternative to incisional strabismus surgery.
22.) Oculinum injection-resistant blepharospasm in young patients.
23.) Botulinum A chemodenervation: a new modality in cerebral palsied hands.
24.) Botulinum toxin--a possible new treatment for axillary hyperhidrosis.
25.) Local injection into mimetic muscles of botulinum toxin A for the treatment of facial lines.
26.) Long term results of botulinum toxin type A (Dysport) in the treatment of hemifacial spasm: a report of 175 cases.
27.) Contemporary management of the aging brow and forehead.
28.) Botulinum A toxin therapy: neutralizing and nonneutralizing antibodies--therapeutic consequences.
29.) One hundred cases of anal fissure treated with botulin toxin: early and long-term results.
30.) Botulinum A toxins: units versus units.
31.) Reconstituted botulinum toxin type A does not lose potency in humans if it is refrozen or refrigerated for 2 weeks before use.
32.) [Mechanism of action, clinical indication and results of treatment of botulinum toxin]
33.) Use of botulinum toxin in stroke patients with severe upper limb spasticity.
34.) Nerve injection injury with botulinum toxin.
35.) DYSBOT: a single-blind, randomized parallel study to determine whether any differences can be detected in the efficacy and tolerability of two formulations of botulinum toxin type A--Dysport and Botox--assuming a ratio of 4:1.
36.) Patient selection in the treatment of glabellar wrinkles with botulinum toxin type A injection.
37.) Botulinum A neurotoxin for axillary hyperhidrosis. No sweat Botox.
38.) Botox-induced prostatic involution.
39.) Use of botulinum A toxin in patients at risk of wound complications following eyelid reconstruction.
40.) Cosmetic upper-facial rejuvenation with botulinum.
41.) New Treatment For Sweaty Palms Works for Up To A Year
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1.) Botulinum toxin for chronic anal fissure [see comments]
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CM - Comment in: Lancet 1995 Jan 21; 345(8943):188-9
SO - Lancet 1994 Oct 22;344(8930):1127-8
AU - Gui D; Cassetta E; Anastasio G; Bentivoglio AR; Maria G; Albanese A
AD - Istituto di Clinica Chirurgica, Universita Cattolica del Sacro Cuore, Roma, Italy.
PT - CLINICAL TRIAL; JOURNAL ARTICLE
AB - Botulinum toxin can chemically denervate striated muscle. Botulinum toxin A (15 U) was used to treat ten patients with chronic anal fissure by injection in the internal sphincter. In seven patients, the lesion healed at 2 months after treatment; one relapsed at 3 months. In one patient the lesion healed at 1 month, but partly relapsed a month later. Mild faecal incontinence lasting for 1 day was observed in one patient. We propose that botulinum toxin injections in the internal anal sphincter be considered an alternative approach to surgical therapy of anal fissure.
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2.) Botulinum toxin A for hyperkinetic facial lines: results of a double-blind, placebo-controlled study.
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SO - Plast Reconstr Surg 1994 Jul;94(1):94-9
AU - Keen M; Blitzer A; Aviv J; Binder W; Prystowsky J; Smith H; Brin M
AD - Department of Otolaryngology, Columbia University College of Physicians and Surgeons, New York, N.Y.
PT - CLINICAL TRIAL; JOURNAL ARTICLE; RANDOMIZED CONTROLLED TRIAL
AB - Previous work on patients with muscular dystonia has shown that small intramuscular doses of botulinum toxin A eliminated hyperkinetic facial lines for approximately 6 months. The purpose of this study was to determine the efficacy of botulinum toxin A injections in eliminating facial wrinkles in aesthetic surgery patients who do not have muscular dystonia. Eleven healthy subjects were studied in a double-blind fashion. On both sides of the face, 0.2 cc of either normal saline or botulinum toxin A was injected into the forehead or into the periorbital wrinkles (crow's feet). Documentation of results was made by photographs taken of the patients during repose and during facial animation before and after injection. Assessment of facial wrinkles was done from a grading system in which the patient and the facial plastic surgeon were asked to judge the severity of the wrinkles on a scale from 0 to 3, with 0 reflecting no facial wrinkles and 3 reflecting severe facial wrinkling. Nine of 11 subjects injected with botulinum toxin A noted a significant improvement in the severity of their facial wrinkles in comparison with the side of the face injected with saline, with a rating improvement of 2 points. Two of 11 subjects noted a moderate improvement, with a rating improvement of 1 point. No patient injected with saline reported an improvement in the severity of the facial wrinkles on the control side. There were no serious complications. Botulinum toxin A is an efficacious method of nonsurgically eliminating facial wrinkles and may play a role in the cosmetic enhancement of the aging face.
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3.) Botulinum toxin for the treatment of hyperfunctional lines of the face [see comments]
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CM - Comment in: Arch Otolaryngol Head Neck Surg 1995 Jun; 121(6):704
SO - Arch Otolaryngol Head Neck Surg 1993 Sep;119(9):1018-22
AU - Blitzer A; Brin MF; Keen MS; Aviv JE
AD - Department of Otolaryngology, Columbia-Presbyterian Medical Center, New York, NY.
PT - JOURNAL ARTICLE
AB - OBJECTIVE: To determine the effectiveness of botulinum toxin injections for the management of hyperfunctional facial lines in patients with dystonia. DESIGN: Twenty-six patients were included in the study: 24 patients had dystonic movement of the face as either a primary or secondary component, and two patients were treated for purely hyperfunctional lines. Botulinum toxin type A was injected via a monopolar hollow-bore Teflon-coated electromyography needle into the facial muscles associated with the hyperfunctional lines. Doses were divided into 1.25- to 10-U aliquots. Qualitative assessments by the patient and physician were made before injection and 2 to 3 weeks after injection. PATIENTS: Twenty-six patients (two male and 24 female) with hyperfunctional lines were included. The ages were from 32 to 84 years with an average age of 59 years. Twenty had dystonia, four had hemifacial spasm, and two had pure hyperfunction without neuromuscular disease. RESULTS: All of the patients had an effect of toxin within the first 24 to 72 hours. All of the patients experienced benefit from the toxin injections with partial or total resolution of painful contractions or unsightly hyperfunctional lines and spasms. The effects of the injection lasted 3 to 6 months. No systemic side effects were noted. Adverse effects included mild, temporary eyelid or lip weakness. CONCLUSION: Based on this initial pilot study, botulinum toxin may be an important new option for the treatment of patients with hyperfunctional facial lines.
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4.) Spasmodic dysphonia. Emotional status and botulinum toxin treatment.
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SO - Arch Otolaryngol Head Neck Surg 1994 Mar;120(3):310-6
AU - Murry T; Cannito MP; Woodson GE
AD - Department of Otolaryngology-Head and Neck Surgery, University of Tennessee College of Medicine, Memphis.
PT - JOURNAL ARTICLE
AB - The objectives of this study were to determine the effects of botulinum toxin injection on measures of depression, anxiety, and somatic complaints in patients diagnosed as having spasmodic dysphonia. Patients were asked to complete preinjection questionnaires with self-ratings of depression, state and trait anxiety, and somatic complaints. Approximately 1 week and 2 months following injection, patients were again asked to complete the questionnaires. The spasmodic dysphonic subjects exhibited significantly elevated mean levels of depression and anxiety. These levels were significantly reduced approximately 1 week after injection. Two months later, depression and anxiety measures did not change significantly from their 1-week postinjection values. The results suggest that patients with spasmodic dysphonia who demonstrate significantly elevated measures of depression and anxiety show a reduction in those measures following treatment with botulinum toxin.
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5.) Botulinum A toxin for treatment of aberrant facial nerve regeneration.
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SO - Plast Reconstr Surg 1993 May;91(6):1042-5
AU - Borodic GE; Pearce LB; Cheney M; Metson R; Brownstone D; Townsend D; McKenna M
AD - Department of Ophthalmology and Otolaryngology, Massachusetts Eye and Ear Infirmary, Boston.
PT - JOURNAL ARTICLE
AB - Twelve patients with involuntary synkinetic eyelid closure were given 40 injections of botulinum A toxin. Temporary improvement in involuntary eyelid closure was observed in all 12 patients. Eleven of the 12 patients desired repeated injections. Dose requirements for this indication were compared with doses used in 697 injections in 112 patients with essential blepharospasm and Meige syndrome. Additionally, dose comparisons were made with 269 injections in 71 patients with hemifacial spasm. Dose requirements needed to treat aberrant regeneration of the facial nerve were substantially less than needed to treat blepharospasm and Meige syndrome. The dose requirement was similar to that in hemifacial spasm treatment. The reason for the differences probably relates to existing muscular denervation associated with hemifacial spasm and aberrant facial nerve regeneration.
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6.) Crystalline preparation of botulinum toxin type A (Botox): degradation in potency with storage [see comments]
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CM - Comment in: Otolaryngol Head Neck Surg 1993 Nov; 109(5):968-9
SO - Otolaryngol Head Neck Surg 1993 Feb;108(2):135-40
AU - Gartlan MG; Hoffman HT
AD - Department of Otolaryngology-Head and Neck Surgery, University of Iowa Hospitals and Clinics, Iowa City 52242.
MJ - Botulinum Toxins
MN - Biological Assay; Drug Storage [methods]; Freeze Drying; Mice, Inbred Strains; Mice; Time Factors
MT - Animal; Female
PT - JOURNAL ARTICLE
AB - Laryngeal injection of botulinum toxin type A is currently the most effective method of treating spasmodic dysphonia. Botox, a crystalline preparation of botulinum toxin type A, is the only toxin approved for clinical use in the United States and is packaged in vials of 100 mouse units (MU). One MU corresponds to the calculated median lethal intraperitoneal dose (LD50) injected in mice. The logistic problems arising from the need for repeated injections of small amounts of Botox have been addressed by several investigators by refreezing unused Botox for use at a later time. Although FDA labeling recommends that Botox not used within 4 hours of reconstitution be discarded, data regarding degradation in potency after reconstitution and refreezing are not currently available. Using the LD50 Swiss-Webster mouse bioassay and statistical analysis by the Probit procedure, a 69.8% loss in potency was found when Botox was reconstituted, immediately frozen, and then assayed 2 weeks later (p 0.0001). Statistically significant degradation in potency was seen after refrigerator storage for 12 hours (p = 0.007), but not for 6 hours (p = 0.16). Clinical implications regarding the dilution, use, and storage of Botox are discussed.
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7.) Botulinum toxin. From poison to medicine.
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SO - West J Med 1993 Jan;158(1):25-9
AU - Davis LE
AD - Neurology Service, Veterans Affairs Medical Center, Albuquerque, NM 87108.
PT - JOURNAL ARTICLE; REVIEW (56 references); REVIEW, TUTORIAL
AB - Although thousands of people in the world each year continue to be poisoned with botulinum toxin-food-borne, infantile, or wound botulism-the neurotoxin is now sufficiently understood to allow it to be used as a medicinal agent to paralyze specific muscles, giving temporary symptomatic relief from a variety of dystonic neurologic disorders. I review some of the epidemiologic, clinical, and pathophysiologic aspects of botulinum toxin and how the neurotoxin may act as a poison or a medicine.
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8.) Botulinum B toxin as an alternative to botulinum A toxin: a ======================================================================
histologic study.
SO - Ophthal Plast Reconstr Surg 1993;9(3):182-90
AU - Borodic GE; Pearce LB; Smith KL; Phelan M; Ferrante R
AD - Boston University School of Medicine, University Hospital, Massachusetts.
PT - JOURNAL ARTICLE
AB - Histochemical effects of botulinum B toxin were studied on fibers from longissimus dorsi muscle in Albino rabbits and compared to effects produced by botulinum A toxin. Acetylcholinesterase staining, muscle fiber size analysis, and ATPase staining indicated botulinum B toxin produced a denervation gradient and field similar to that produced by botulinum A toxin. At 5 weeks postinjection with botulinum B toxin, analysis showed muscle fiber size variability, and diffuse acetylcholinesterase fiber staining comparable to botulinum A toxin at the injection site. Muscle sections taken at 4.0 cm for analysis showed statistically significant decreased fiber size variability and contraction of acetylcholinesterase staining pattern for both immunotypes. In addition, the denervation reflected by histochemical staining and fiber size analysis appeared transient and lasted for approximately 3 months for both immunotypes. These findings suggest botulinum B toxin produces pharmacologic effects on innervation of striated muscle similar to botulinum A toxin. Because immunologic tolerance has been demonstrated after therapeutic botulinum A toxin injections, further clinical studies need to be conducted with other immunotypes of toxin with no cross-reactivity to type A.
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9.) Psoriasiform eruption from intramuscular botulinum A toxin.
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SO - Cutis 1992 Dec;50(6):415-6
AU - Bowden JB; Rapini RP
AD - Department of Dermatology, University of Texas Medical School, Houston 77030.
PT - JOURNAL ARTICLE
AB - Botulinum A toxin is used intramuscularly in the treatment of spastic neuromuscular disorders, strabismus, and laryngeal dystonia. The toxin has recently been reported as being useful for the cosmetic removal of glabellar furrows. The clinical effect of the toxin lasts four months or longer. Systemic side effects are rare and usually transient. We report the case of a psoriasiform eruption temporally related to the injection of botulinum A toxin into the medial rectus muscle to treat an ocular motility disorder. To our knowledge, this is the first case of a psoriasiform dermatitis caused by this agent.
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10.) Contralateral injections of botulinum A toxin for the treatment of hemifacial spasm to achieve increased facial symmetry [see comments]
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CM - Comment in: Plast Reconstr Surg 1993 Dec; 92(7):1409
SO - Plast Reconstr Surg 1992 Dec;90(6):972-7; discussion 978-9
AU - Borodic GE; Cheney M; McKenna M
AD - Massachusetts Eye and Ear Infirmary, Boston.
PT - JOURNAL ARTICLE
AB - Six patients noted facial asymmetry after botulinum toxin injection for hemifacial spasm. Each patient was injected on the side contralateral to the spasms with 10 to 15 IU over the zygomatic major and minor muscles. Each patient noted improvement in facial symmetry in the resting position and dynamic facial movements. Five of the six patients desired this approach with subsequent injections. This injection method variation proved helpful in the managing of hemifacial weakness created by botulinum A toxin for this condition.
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11.) Clinical and laboratory comparison of botulism from toxin types A, B, and E in the United States, 1975-1988.
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SO - J Infect Dis 1992 Dec;166(6):1281-6
AU - Woodruff BA; Griffin PM; McCroskey LM; Smart JF; Wainwright RB; Bryant RG; Hutwagner LC; Hatheway CL
AD - Enteric Diseases Branch, Centers for Disease Control, Atlanta, Georgia 30333.
PT - JOURNAL ARTICLE
AB - Cases of adult botulism (n = 309) were studied to identify clinical differences between toxin types and to evaluate the sensitivity of diagnostic laboratory testing. Patients with illness from type E toxin had the shortest incubation periods. Sporadic case-patients were more severely ill: 85% required intubation compared with only 42% in multiperson outbreaks. Of patients with type A botulism, 67% required intubation compared with 52% with type B and 39% with type E. Toxin testing was positive for 40%-44% of serum and stool specimens obtained within 3 days of toxin ingestion and for 15%-23% of specimens obtained thereafter, while 37% of stool specimens obtained 3 days after toxin ingestion were positive by culture. Patients with type A botulism have more severe illness. In general, specimens obtained early are more likely to be positive by toxin assay, and stool cultures are more sensitive than toxin detection for specimens obtained later in the illness.
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12.) Treatment of glabellar frown lines with C. botulinum-A exotoxin.
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SO - J Dermatol Surg Oncol 1992 Jan;18(1):17-21
AU - Carruthers JD; Carruthers JA
AD - Department of Opthalmology, University of British Columbia, Vancouver, Canada.
PT - JOURNAL ARTICLE
AB - Eighteen patients with glabellar frown lines were treated with C. botulinum-A exotoxin. Sixteen of the 17 patients followed showed improvement for periods ranging from 3 months to 11 months. Side-effects were minimal and transient. Because C. botulinum-A exotoxin therapy of glabellar frown lines treats the underlying cause of these lines, it is more effective than soft tissue augmentation although this improvement is temporary. Treatment with C. botulinum-A exotoxin is a simple, safe procedure.
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13.) Botulinum A toxin for (expressionistic) ptosis overcorrection after frontalis sling.
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SO - Ophthal Plast Reconstr Surg 1992;8(2):137-42
AU - Borodic GE
AD - Gunderson Eye Clinic, Boston University, Massachusetts Eye and Ear Infirmary, Boston 02114.
PT - JOURNAL ARTICLE
AB - Botulinum A toxin was injected into the frontalis muscle in two patients with complete third nerve palsies to limit intermittent upper lid retraction after a frontalis sling procedure. This form of lid retraction is noted during periods of active facial movement with occipitofrontalis muscle contraction. Although upper lid position may be symmetric when the facial muscles are adynamic, the upper lid may retract during periods of active facial expression. This type of lid retraction was corrected using Botulinum A toxin injections into the frontalis muscles, without affecting the lid position when the facial muscles are adynamic. Both improvement in appearance and intermittent exposure were noted in both cases. Additionally, a blunting of the transverse forehead creases occurred over a defined area after this injection, representing a clinical example of a denervation field produced by a point injection of botulinum toxin.
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14.) Botulinum A toxin for the treatment of adult-onset spasmodic torticollis.
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SO - Plast Reconstr Surg 1991 Feb;87(2):285-9
AU - Borodic GE; Mills L; Joseph M
AD - Massachusetts Eye and Ear Infirmary, Boston.
PT - JOURNAL ARTICLE
AB - Thirty-five patients with adult-onset idiopathic torticollis were treated by local injections of botulinum A toxin into dystonic cervical muscles. Substantial improvement with respect to reduction and elimination of pain was found in 81 percent, improvement in posture deformity and involuntary spasms in 70 percent, increased range of motion of the neck in 78 percent, reduction in visible sternocleidomastoid hypertrophy in 86 percent, and improvement in tremor in 65 percent. The syndrome was divided into four subtypes based on pattern of dystonic muscle groups involved in the dystonia, head and shoulder posture, and sternocleidomastoid muscle hypertrophy. Injection strategy based on this subdivision is described.
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15.) Treatment of idiopathic spasmodic torticollis with botulinum-A toxin: a pilot study of 19 patients.
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SO - Med J Aust 1990 May 21;152(10):528-30
AU - Lorentz IT; Subramaniam SS; Yiannikas C
AD - Westmead Hospital, NSW.
PT - JOURNAL ARTICLE
AB - Nineteen patients with spasmodic torticollis, unresponsive to standard therapy, were administered local injections of botulinum-A toxin into the affected muscles. During an average follow-up period of 11.5 months, a more than 25% improvement was noted in 14 of 19 patients. All those with purely focal dystonia and 9 of 10 patients with a disease history of less than three years benefited from treatment. Side effects were insignificant and transient. Botulinum toxin is a very effective and safe method of treatment for spasmodic torticollis.
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16.) Botulinum A toxin injection. Failures in clinical practice and a
biomechanical system for the study of toxin-induced paralysis.
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SO - Ophthal Plast Reconstr Surg 1990;6(4):252-9
AU - Holds JB; Fogg SG; Anderson RL
AD - Department of Ophthalmology, Bethesda Eye Institute, St. Louis University School, Missouri 63110.
PT - JOURNAL ARTICLE
AB - Botulinum A toxin injection has great utility in the treatment of essential blepharospasm and other facial spasm disorders. Several investigators have noted the failure of botulinum toxin injections to relieve lid spasm in occasional patients and a decrease in effectiveness or duration of effect following multiple injections in other patients. We reviewed the charts of 30 consecutive patients presenting for the evaluation or treatment of facial dystonia. Of 20 patients who had received multiple injections of botulinum toxin, 10 patients were felt to be treatment failures. A new biomechanical system was developed to investigate the duration and degree of paralysis induced in the gastrocnemius muscle of the rat. Animals were treated with four sequential injections at 6-week intervals to the same muscle, resulting in muscle atrophy and an increase in the duration and degree of muscle paralysis, contrary to clinical findings in humans. The review of patient data confirms that, for many patients, repeated injection of botulinum toxin results in a decrease in duration and degree of effect despite an increased toxin dose. An opposite effect was noted in our experimental model because of progressive muscle atrophy.
======================================================================
17.) Treatment of blepharospasm with botulinum toxin.
======================================================================
SO - Mayo Clin Proc 1989 Sep;64(9):1085-90
AU - Kennedy RH; Bartley GB; Flanagan JC; Waller RR
AD - Oculoplastic Service, Wills Eye Hospital, Philadelphia, Pennsylvania.
PT - JOURNAL ARTICLE
AB - Many therapeutic modalities, including medications, excision of the muscles used in closure of the eyelids (myectomy), and selective extirpation of branches of the facial nerve (neurectomy), have been used for the management of blepharospasm. Because of limited effectiveness and undesirable side effects, none of these treatments has been completely satisfactory. Recent reports about injection of botulinum toxin indicate that it is safe and effective for most patients. Relief from blepharospasm, however, is usually transient, and repeated injections are usually necessary. The current availability of effective therapy for blepharospasm emphasizes the importance of prompt diagnosis and referral of affected patients to physicians knowledgeable in the use of botulinum toxin and other therapeutic approaches.
======================================================================
18.) Botulinum toxin: a treatment for facial asymmetry caused by facial nerve paralysis.
======================================================================
SO - Plast Reconstr Surg 1989 Aug;84(2):353-5
AU - Clark RP; Berris CE
AD - Section of Plastic and Reconstructive Surgery, Mercy General Hospital, Sacramento, Calif.
PT - JOURNAL ARTICLE
AB - Injury to the frontal or other facial nerve branches can result in an asymmetry that can be very distressful to both patient and surgeon. This is especially true following cosmetic procedures such as rhytidectomy. We propose a means to create temporary symmetry while awaiting the possible return of nerve function. Botulinum neurotoxin causes a muscle paralysis lasting for approximately 3 months, and it is well established as the preferred treatment for blepharospasm. A case is presented in which botulinum toxin type A was injected into the opposite functioning frontalis muscle of a patient with unilateral frontal nerve paralysis. The patient experienced satisfactory relief of the asymmetry caused by onesided forehead wrinkling and brow elevation. Botulinum toxin therapy should be considered for both temporary and permanent facial asymmetries due to facial nerve paralysis as well as spasm.
======================================================================
19.) Management of facial spasm with Clostridium botulinum toxin, type A (Oculinum) [see comments]
======================================================================
CM - Comment in: Arch Otolaryngol Head Neck Surg 1989 Jul; 115(7):882
SO - Arch Otolaryngol Head Neck Surg 1988 Dec;114(12):1407-12
AU - Biglan AW; May M; Bowers RA
AD - Department of Ophthalmology, University of Pittsburgh School of Medicine, PA.
PT - JOURNAL ARTICLE; REVIEW (39 references); REVIEW OF REPORTED CASES
AB - One hundred five patients received 391 graded injections of Clostridium botulinum type A toxin (Oculinum) to treat uncontrollable facial muscle spasm. Patients had essential blepharospasm (n = 61), hemifacial spasm (n = 24), or aberrant regeneration of the seventh cranial nerve (n = 20). Muscle spasms were reduced within two days of the first injection of toxin and, in most cases, the drug effect lasted three to four months. Control of facial muscle spasm was achieved in all patients. Complications related to treatment included transient blepharoptosis (n = 7), diplopia (n = 2), and altered facial expression (n = 11). Systemic side effects were not observed. Select chemodenervation of facial muscles with graded injections of botulinum toxin is a useful adjunct to control blepharospasm, hemifacial spasm, and facial spasm due to aberrant regeneration of the facial nerve.
======================================================================
20.) Treatment of anismus in intractable constipation with botulinum A toxin.
======================================================================
SO - Lancet 1988 Sep 24;2(8613):714-7
AU - Hallan RI; Williams NS; Melling J; Waldron DJ; Womack NR; Morrison JF
AD - Surgical Unit, London Hospital, Whitechapel.
PT - JOURNAL ARTICLE
AB - In seven patients with anismus the striated sphincter muscle complex was selectively weakened by local injection of Clostridium botulinum type A toxin. Symptom scores improved significantly and correlated with a significant reduction in the maximum voluntary and canal squeeze pressure and a significant increase in the anorectal angle on straining. Botulinum A toxin seems to be promising treatment for some patients with anismus.
EM - 8812
======================================================================
21.) Botulinum toxin chemodenervation in infants and children: an
alternative to incisional strabismus surgery.
======================================================================
SO - J Pediatr 1987 May;110(5):719-22
AU - Magoon E; Scott AB
MJ - Botulinum Toxins; Oculomotor Muscles [innervation]; Strabismus [therapy]
MN - Child, Preschool; Child; Denervation [methods]; Electromyography; Infant; Ketamine
MT - Human; Support, Non-U.S. Gov't; Support, U.S. Gov't, P.H.S.
PT - JOURNAL ARTICLE
AB - Eighty-two children aged 13 years or younger were given injections of botulinum toxin for horizontal strabismus. Improvement was achieved in all but one patient. Children younger than 1 year or older than 6 years of age received only topical drop anesthesia and no sedation. Young children generally required low-dose ketamine sedation. The technique typically undercorrects, so reinjection was necessary in 85% of the patients. There were no systemic complications. Side effects, lasting up to a few weeks, included transient ptosis and hypertropia caused by involvement of other extraocular muscles.
======================================================================
22.) Oculinum injection-resistant blepharospasm in young patients.
======================================================================
SO - Ophthal Plast Reconstr Surg 1994 Sep;10(3):193-4
AU - Gausas RE; Lemke BN; Sherman DD; Dortzbach RK
AD - Department of Ophthalmology, University of Wisconsin-Madison 53792-3220.
PT - JOURNAL ARTICLE
AB - Botulinum toxin has recently been used as a nonsurgical treatment for blepharospasm and other facial dyskinesias. This report describes four patients between the ages of 32 and 37 years who failed to respond to botulinum injections for severe blepharospasm. Other than age, no other features could be identified in these patients that would differentiate this group. Particularly early age of onset for essential blepharospasm might be an indicator of failure to respond to the injections.
======================================================================
23.) Botulinum A chemodenervation: a new modality in cerebral palsied hands.
======================================================================
SO - Br J Plast Surg 1993 Dec;46(8):703-6
AU - Wall SA; Chait LA; Temlett JA; Perkins B; Hillen G; Becker P
AD - Division of Plastic and Reconstructive Surgery, University of the Witwatersrand, South Africa.
PT - JOURNAL ARTICLE
AB - Botulinum A chemodenervation of the Adductor Pollicis muscle for the treatment of the thumb-in-palm deformity in cerebral palsied hands is presented as a new therapeutic option. Early results of a clinical trial in five hemiparetic Cerebral Palsied (C.P.) children are assessed using a prospective nontrialist-biased study design based on an independent panel assessment of pre- and post-intervention photographic and videotaped records of hand function and appearance, in combination with grip dynamometry and goniometry. All cases are shown to improve in terms of both function and appearance with results approaching statistical significance (p = 0.06) when assessed by the Wilcoxon's matched-pairs signed rank test, despite the small study group. The modality is shown to be simple, safe and effective over the period reported (229 days). The benefit is sustained beyond the period of muscle paresis and ongoing long term follow-up will document the need for, and timing of, reinjection.
======================================================================
24.) Botulinum toxin--a possible new treatment for axillary hyperhidrosis.
======================================================================
Author
Bushara KO; Park DM; Jones JC; Schutta HS
Address
Department of Neurology, University of Wisconsin Hospital and Clinics, Madison
53792-5132, USA.
Source
Clin Exp Dermatol, 21(4):276-8 1996 Jul
Abstract
The inhibitory action of botulinum toxin is not limited to the neuromuscular junction. The toxin
also blocks the autonomic cholinergic fibres, including the sympathetic fibres to sweat glands.
We have previously demonstrated that the toxin produces localized anhidrosis. To determine
the dosage, pattern and duration of the anhidrotic effect of botulinum toxin and to test the
efficacy of axillary injections, we further studied seven healthy volunteers. Two individuals
had subcutaneous injections of botulinum toxin (20 mouse units, Dysport-Porton Products) in
the dorsum of the hand. Five healthy volunteers had 15-50U of botulinum toxin A (Botox)
injected in one axilla. A circular area of complete anhidrosis on the dorsum of the hand was
evident on day 2 and persisted for 11 months. By day 3, two of the axillae (injected with 50
U each) were totally dry and in one (injected with 30 U) the sweating was substantially
reduced. The effect persisted for 6-8 months before wearing off. No effect was appreciated
in two axillae (injected with 15 and 20 U). No significant side-effects were encountered.
Subcutaneous injections of botulinum toxin causes chemodenervation of the sweat glands. In
normal individuals axillary sweating can be abolished by 50 U of botulinum toxin A (Botox).
The results offer a possible novel treatment for severe cases of axillary hyperhidrosis.
Language
Eng
======================================================================
25.) Local injection into mimetic muscles of botulinum toxin A for the treatment of facial lines.
======================================================================
Author
Guerrissi J; Sarkissian P
Address
Service of Plastic Surgery, Argerich Hospital, Buenos Aires, Argentina.
Source
Ann Plast Surg, 39(5):447-53 1997 Nov
Abstract
The purpose of this clinical investigation is to confirm the efficacy of eliminating facial wrinkles
by injecting botulinum toxin A into mimetic muscles. Fifty-four patients were injected with
BOTOX A-14 in the corrugator superciliaris, 19 in the frontalis muscles, and 13 in the
orbicularis oculis. Dilution was obtained by adding 4 ml preservative-free saline to 100 IU of
BOTOX A. The dose used varied according to the patient. The severity of wrinkles and the
intensity of muscle contraction (facial expression) were taken into account. The paralysis
obtained in the mimetic muscles was effective for 6 months in 39 patients, 8 months in 10
patients, and 9 months in 1 patient. The results were documented by photographs, videotape,
and electromyographies pre- and postinjection. To preserve the results, 21 patients (39%)
demanded a second infiltration to achieve satisfactory results. Neither local nor general
adverse effects were noted, except transitory eyebrow palsy in 2 patients, and edema and
ecchymosis in 4 patients. The improvement obtained in facial mimetic wrinkles was
satisfactory to the patient and to us.
======================================================================
26.) Long term results of botulinum toxin type A (Dysport) in the treatment of hemifacial spasm: a report of 175 cases.
======================================================================
Author
Jitpimolmard S; Tiamkao S; Laopaiboon M
Address
Department of Medicine, Faculty of Medicine, Khon Kaen University, Thailand.
Suthip-J@Medlib2.kku.ac.th
Source
J Neurol Neurosurg Psychiatry, 64(6):751-7 1998 Jun
Abstract
OBJECTIVE: To describe the long term efficacy and side effects of the treatment of
hemifacial spasm with Dysport and to evaluate two different sites of injection to hopefully
reduce side effects. METHODS: This study was designed as a prospective descriptive study.
Injections were made subcutaneously around the eye. Peak improvement was subjectively
assessed by using a visual analogue scale and reported in percentages (0-100%). Duration of
improvement was assessed subjectively and reported in months. RESULTS: Of 175 cases,
17 were lost to follow up and were excluded. 855 treatments were injected in the remaining
158 patients with a median of 4 treatments. The response rate was 97%. Of 855 treatments,
the adjusted mean peak and duration of improvement was 77.2 (95% confidence interval
(95%CI) 74.7-79.4)% and 3.4 (95%CI 3.2-3.6) months respectively. In 158 patients
(complete group), the long term results from the first to the 12th treatment showed that the
mean peak improvement ranged from 72.70 to 80.10% and the duration of improvement
was 2.60 to 3.71 months. It remained constant throughout (p=0.40, p=0.87 respectively).
The most common side effect was ptosis. Of the 158 patients, 21 completed 12 treatments
(subgroup). A separate analysis of this group disclosed a mean peak and duration of
improvement from the first to 12th treatments ranging from 70.00 to 78.10% and 2.65 to
4.31 months respectively. Analysis of variance with repeated measures showed no significant
variation of peak and duration of improvement over the first to the 12th treatments (p=0.38,
p=0.38 respectively). Only 3% of the treatments were unsuccessful but responded to
subsequent treatments. The incidence of ptosis was reduced from 27.17% to 9.68% by
moving the injection site to the lateral part of orbital orbicularis oculi without any loss of
efficacy. The yearly cost of Dysport is considerably less than Botox. CONCLUSION: This
study is the first to show, in detail, the long term results of treatments of hemifacial spasm with
Dysport. The efficacy is constant throughout orbicularis oculi. The efficacy of Dysport is
comparable with Botox in long term follow up.
======================================================================
27.) Contemporary management of the aging brow and forehead.
======================================================================
Author
Koch RJ; Troell RJ; Goode RL
Address
Division of Otolaryngology-Head and Neck Surgery, Stanford University, California
94305-5328, U.S.A.
Source
Laryngoscope, 107(6):710-5 1997 Jun
Abstract
Management of the aging brow and forehead has recently evolved based on available
innovative technologies. Likewise, procedure-specific indications have changed based on
collective surgical experiences. No longer is the approach based solely on hair pattern or
degree of brow ptosis. Patients require varying combinations of brow elevation (prior to
blepharoplasty), correction of brow asymmetries, and hairline-preserving forehead elevation.
Some may only require excisional or paralytic procedures of the frontalis muscle (horizontal
forehead creases), corrugator supercilii muscles (vertical glabellar furrows), and procerus
muscle (horizontal glabellar furrows). We present a 3-year experience using a
problem-specific approach. This incorporates endoscopic technology, botulinum toxin type A
purified neurotoxin complex (Botox, Allergan, Irvine, CA) intramuscular injection, and
traditional procedures such as the coronal, pretrichial, midforehead, and direct browlift.
Current indications, patient selection, and results are also discussed.
======================================================================
28.) Botulinum A toxin therapy: neutralizing and nonneutralizing antibodies--therapeutic consequences.
======================================================================
Author
G¨oschel H; Wohlfarth K; Frevert J; Dengler R; Bigalke H
Address
Institute of Toxicology, Medical School of Hannover, Germany.
Source
Exp Neurol, 147(1):96-102 1997 Sep
Abstract
Although muscle-relaxant doses of botulinum A toxin (BoNT/A) are generally lower than
doses stimulating the immune system, specific antibodies are raised in a substantial number of
patients. As a rule, this necessitates the termination of treatment. Therefore, a reliable
determination of specific anti-BoNT/A antibodies is helpful and we introduced, for this
purpose, a novel in vitro toxin-neutralizing assay based on a nerve-muscle preparation. We
measured the antibody titers in four groups of subjects: Group 1 comprised 75 randomly
selected patients of a total of 295 who responded to treatment with Dysport in our local
clinic. Five patients, in group 2, were nonresponders. Group 3 consisted of 32 untreated
volunteers and group 4 of 8 subjects immunized with a toxoid more than 10 years ago. Two
of the responders had marginal titers of neutralizing antibodies, while they were present in all
nonresponders. The sera of all responders were also tested for nonneutralizing antibodies by
ELISA. Their occurrence, however, was of no consequence to the therapeutic success. The
blood samples of volunteers were free from specific antibodies, whereas antibodies persisted
in the immunized subjects for longer than a decade. Patients from various clinics who had
been treated unsuccessfully with the toxin-14 patients had received BOTOX, 7 had been
treated with Dysport, and 7 with both products-all had neutralizing antibodies. Whether there
was an antibody response depended on the amount of toxin administered. We believe,
however, the effective toxin dose can be reduced by so much as to make antibody
production highly improbable.
======================================================================
29.) One hundred cases of anal fissure treated with botulin toxin: early and long-term results.
======================================================================
Author
Jost WH
Address
Department of Neurology and Clinical Neurophysiology, Deutsche Klinik f¨ur Diagnostik,
Wiesbaden, Germany.
Source
Dis Colon Rectum, 40(9):1029-32 1997 Sep
Abstract
PURPOSE: Sphincterotomy still is considered the therapy of choice to eliminate sphincter
spasm in the treatment of uncomplicated chronic anal fissure. The surgery is weighted with the
possible surgical risk and the risk of subsequent fecal incontinence. This study reports the
effect of botulin toxin injections within the first six months. PATIENTS AND METHODS:
One hundred patients were treated (43 females; average age, 34.7 years). The injection of
botulin toxin (2.5-5 units of Botox each) was done bilaterally to the fissure, thereby causing
paresis of the sphincters for approximately three months. Patients were re-examined after one
week and three and six months. RESULTS: Within the first week, 78 percent of patients
were free of pain. In 82 percent of patients, complete healing of the fissure occurred within
the first three months. Eight patients experienced relapses within the first six months of
therapy, three of whom needed surgical intervention. The healing rate after six months was 79
percent. No healing occurred in 21 patients, and they had to undergo surgery. Transitory
fecal incontinence resulted in seven cases. CONCLUSIONS: Injection of botulin toxin
enables us to treat chronic, uncomplicated anal fissures with increased sphincter tone. It is
well tolerated, can be administered on an outpatient basis, does not cause any lesion of the
continence organ, and subsequently, does not lead to any permanent latent or apparent fecal
incontinence.
======================================================================
30.) Botulinum A toxins: units versus units.
======================================================================
Author
Wohlfarth K; G¨oschel H; Frevert J; Dengler R; Bigalke H
Address
Department of Neurology, Medical School of Hannover, Germany.
Source
Naunyn Schmiedebergs Arch Pharmacol, 355(3):335-40 1997 Mar
Abstract
We investigated the efficacies and potencies of two commercial preparations of botulinum
neurotoxin type A (BoNt/A) reputed to differ in potency. Tests were conducted in vitro using
the mouse phrenic nerve-hemidiaphragm which is an approved tool for measuring clostridial
toxicity. In addition, in a double-blind trial on volunteers, varying amounts of one product
were injected into the Musculus extensor digitorum brevis of the left foot, while equal
amounts, i.e. units, of the other preparation were injected into the same muscle of the right
foot. Compound muscle action potentials (CMAPs) were recorded before and at various
points in time after the injections. As opposed to wide-spread anecdotal reports, no
difference in effectiveness was found. The dose-response curves obtained from the mouse
organ preparation with both commercial products equalled one another in potency (number
of units) and corresponded to previous toxicity tests in mice conducted elsewhere.
Dose-response curves from volunteers were also identical for both commercial preparations.
The time course of paralysis and recovery of muscle function did not differ either. At lower
concentrations of toxin, however, restoration of muscle function was more rapid than at
higher concentrations. Since the results obtained from man and the animal organ preparation
are in excellent accord, we conclude that 1 unit of Botox corresponds to 1 unit of Dysport.
======================================================================
31.) Reconstituted botulinum toxin type A does not lose potency in humans if it is refrozen or refrigerated for 2 weeks before use.
======================================================================
Author
Sloop RR; Cole BA; Escutin RO
Address
Department of Neurology, Loma Linda University School of Medicine, CA, USA.
Source
Neurology, 48(1):249-53 1997 Jan
Abstract
Botulinum toxin type A (BTX-A) (Botox, Allergan, Irvine, CA) labeling recommends its use
within 4 hours of reconstitution. Since BTX-A is available only in 100-unit vials, a substantial
quantity is often discarded. Using eight volunteers, we measured the percent decline in
extensor digitorum brevis (EDB) M-wave amplitude (percent paralysis) following injection of
freshly reconstituted BTX (right EDB) and compared this with the decline following injection
of BTX that was refrozen (-20 degrees C) or refrigerated (+4 degrees C) for 2 weeks (left
EDB) after reconstitution. When analyzed as paired data, there was essentially no difference
in the muscle paralysis resulting from fresh BTX compared with refrozen or refrigerated BTX,
and no statistical difference between groups was noted. Reconstituted BTX-A that is
subsequently refrigerated or refrozen for 2 weeks does not lose potency in humans.
======================================================================
32.) [Mechanism of action, clinical indication and results of treatment of botulinum toxin]
======================================================================
Author
Lagueny A; Burbaud P
Address
Service de neurologie, h^opital Haut-L´ev´eque, CHRU Bordeaux, Pessoc.
Source
Neurophysiol Clin, 26(4):216-26 1996
Abstract
Botulinum toxin, the most potent of the neurotoxins, produces paralysis by blocking
presynaptic release of the neurotransmitter (acetylcholine) at the neuromuscular junction, with
reversible chemical denervation of the muscle fibre, thereby inducing partial paralysis and
atrophy. Because chemical denervation is reversible, botulinum toxin has temporary effects,
the muscle being progressively reinnervated by nerve sproutings. Type A botulinum toxin
(Bix-A) is available under two dosage forms: Botox and Dysport. Although the initial clinical
indication was strabismus, subsequent studies have demonstrated the efficacy of Btx-A,
mainly in dystonia, hemifacial spasm and spasticity. However, botulinum toxin has been
successfully used in various other clinical indications. In regard to spasticity associated with
cerebral palsy, Btx-A is a promising treatment requiring a multidisciplinary approach. Btx-A
injections lead to effective reduction of muscle hyperactivity with minor side-effects. They are
painless, even though electromyographic guidance may be required for the injection of deep
muscles. However, the production of antibodies to Btx-A may compromise the effect of
long-term treatment.
======================================================================
33.) Use of botulinum toxin in stroke patients with severe upper limb spasticity.
======================================================================
Author
Bhakta BB; Cozens JA; Bamford JM; Chamberlain MA
Address
Rheumatology and Rehabilitation Research Unit, University of Leeds, UK.
Source
J Neurol Neurosurg Psychiatry, 61(1):30-5 1996 Jul
Abstract
OBJECTIVES--Spasticity can contribute to poor recovery of upper limb function after
stroke. This is a preliminary evaluation of the impact of botulinum toxin treatment on disability
caused by upper limb spasticity after stroke. METHODS--Seventeen patients with severe
spasticity and a non-functioning arm were treated with intramuscular botulinum A neurotoxin
(median age at treatment 54.5 years; median time between onset of stroke and treatment 1.5
years). Baseline and assessments two weeks after treatment were compared to assess
efficacy. The duration of improvement in disability was documented. Outcome measures used
were; passive range of movement at the shoulder, elbow, wrist, and fingers; modified
Ashworth scale to assess spasticity of biceps and forearm finger flexors; an eight point scale
to assess the degree of difficulty experienced by the patient or carer for each functional
problem defined before treatment; the presence of upper limb pain. The biceps, forearm
finger flexors, and flexor carpiulnaris were treated with intramuscular botulinum toxin. Up to a
total dose of 400-1000 mouse units (MU) of Dysport (Speywood) or 100-200 MU of
BOTOX (Allergan) was used in each patient. RESULTS--Functional problems reported by
the patients before treatment were difficulty with cleaning the palm, cutting fingernails, putting
the arm through a sleeve, standing and walking balance, putting on gloves, and rolling over in
bed. Hand hygiene improved in 14 of 17 patients; difficulty with sleeves improved in four of
16; standing and walking balance improved in one of four; shoulder pain improved in six of
nine; wrist pain improved in five of six. Passive range of movement at shoulder, elbow, and
wrist improved after treatment. Benefit was noted within two weeks and lasted one to 11
months. No adverse effects occurred. CONCLUSION--This preliminary study suggests that
intramuscular botulinum toxin is a safe and effective treatment for reducing disability in
patients with severe upper limb spasticity.
Language
======================================================================
34.) Nerve injection injury with botulinum toxin.
======================================================================
Author
Lu L; Atchabahian A; Mackinnon SE; Hunter DA
Address
Department of Surgery, Washington University School of Medicine, St. Louis, MO, USA.
Source
Plast Reconstr Surg, 101(7):1875-80 1998 Jun
Abstract
The therapeutic use of botulinum toxin (Botox) is increasing in popularity. Previous studies
have shown that various drugs, especially when injected intrafascicularly, can cause major
nerve damage. This study evaluates the potential for neurotoxicity of botulinum toxin in a rat
sciatic nerve model. Lewis rats were randomly assigned to one of six groups (n = 10/group).
Group 1, 2, and 3 rats received, respectively, an intrafascicular, extrafascicular, and
extraneural injection of 50 microl of botulinum toxin (50 UI/ml). Group 4, 5, and 6 rats
received 50 microl of 10% phenol as a positive control. Five animals received saline as a
negative control. Animals were sacrificed at 2 and 7 weeks. Nerves were harvested and
processed for histology and morphometry. Nerves in all botulinum toxin groups retained a
normal architecture without cellular infiltration or demyelination. The number and diameter of
fibers, the thickness of myelin, and the percentage of neural tissue were comparable with
normal controls. Nerves injected intraneurally with phenol presented with severe damage,
demyelination, and inflammation at 2 weeks and showed signs of early regeneration at 7
weeks. This study demonstrates that in a rat model, even direct intraneural injection of
botulinum toxin caused no damage. This information should encourage the reconstructive
surgeon to consider broader applications of this drug.
======================================================================
35.) DYSBOT: a single-blind, randomized parallel study to determine whether any differences can be detected in the efficacy and tolerability of two formulations of botulinum toxin type A--Dysport and Botox--assuming a ratio of 4:1.
======================================================================
Author
Sampaio C; Ferreira JJ; Sim~oes F; Rosas MJ; Magalh~aes M; Correia AP; Bastos-Lima
A; Martins R; Castro-Caldas A
Address
Institute of Pharmacology and General Therapeutics, Faculty of Medicine, University of
Lisbon, Portugal.
Source
Mov Disord, 12(6):1013-8 1997 Nov
Abstract
BACKGROUND: Elston and Russell discovered a difference in the biological potency of the
English formulation of botulinum toxin type A or BTX-A (Dysport) and the American
formulation (Botox). Potency of both is expressed in LD50 mouse units, but because of
assay differences, these units are not equivalent. Since the first warning by Quinn and Hallet
on the clinical importance of this issue, it has been impossible to reach a consensus on the
conversion factor for the potency of these formulations. OBJECTIVE: To test the hypothesis
that the conversion factor for the clinical potency of Dysport to Botox is approximately 4:1.
DYSBOT is an acronym that results from adding "DYS" from Dysport with "BOT" from
Botox. PATIENTS AND METHODS: Design: A single-blind, randomized, parallel
comparison. A total of 91 patients with blepharospasm or hemifacial spasm were randomized
to treatment with Dysport or Botox using a fixed potency ratio of 4:1. Clinical evaluations:
The patients were evaluated at baseline (day of the treatment). 1 month after treatment, and
whenever the effect was judged to be fading. Objective and functional rating scales were
used as quantitative measures of the change in clinical status. Adverse reactions were
collected using a systematic questionnaire. RESULTS: Using this ratio between products,
both Dysport and Botox groups produced similar clinical efficacy and tolerability. For
patients showing a positive response without the need of a booster, the duration of effect was
13.3 +/- 5.9 weeks for the Dysport group and 11.2 +/- 5.8 weeks for the Botox group. Of
48 patients, 11 (23%) needed booster treatment in the Dysport group compared with five
(12%) of 43 in Botox group. Adverse events were noted in 24 (50%) of 48 patients in the
Dysport group and 20 (47%) of 43 of the Botox-treated group. CONCLUSIONS: Using a
4:1 conversion ratio for Dysport and Botox, similar results were obtained for the two
treatments in an appropriately powered study, suggesting that this conversion factor is a good
estimate of their comparative clinical potencies.
======================================================================
36.) Patient selection in the treatment of glabellar wrinkles with botulinum toxin type A injection.
======================================================================
Author
Pribitkin EA; Greco TM; Goode RL; Keane WM
Address
Department of Otolaryngology-Head & Neck Surgery, Jefferson Medical College,
Philadelphia, Pa, USA.
Source
Arch Otolaryngol Head Neck Surg, 123(3):321-6 1997 Mar
Abstract
OBJECTIVES: To determine the dose-response characteristics and side-effects profile of
Clostridium botulinum type A exotoxin (Botox) used to treat glabellar wrinkles and develop
guidelines for patient selection based on the nature and severity of the treated wrinkles.
DESIGN: Prospective, nonrandomized pilot and electromyogram (EMG)-guided studies.
SETTING: Two ambulatory care clinics at university hospitals. PARTICIPANTS: For the
pilot study, volunteer samples of 23 patients with glabellar wrinkles; for the EMG-guided
study, volunteer samples of 57 patients with glabellar wrinkles. INTERVENTIONS: For the
pilot study, 23 patients were serially injected with up to 10.0 mouse units (MU) of Botox
into each corrugator muscle; for the EMG-guided study, 57 patients were injected under
EMG guidance with an initial dose of 10.0 MU of Botox into each corrugator muscle. Eleven
patients with persistent corrugator activity were reinjected with 10.0 MU of Botox. MAIN
OUTCOME MEASURES: For the pilot study, slide photographs were obtained before and
2 weeks after injection; for the EMG-guided study, slide photographs were obtained before
and at 2 weeks and at 2 months after injection. Patients were asked to evaluate results
numerically. RESULTS: For the pilot study, injection of up to 10.0 MU of Botox into each
corrugator muscle produced a satisfactory improvement in 12 patients; for the EMG-guided
study, 43 patients were satisfied with improvement after full abolition of corrugator or
accessory lateral brow muscle activity. Women were more likely to achieve satisfactory
results than were men (80% [40/50] vs 43% [3/7]; P < or = .03). Improvement was not age
related. No significant side effects or complications were observed. CONCLUSIONS:
Glabellar wrinkles may be satisfactorily treated with Botox injection into the corrugator
supercilii muscles. Improvement is temporary, dose dependent, and may not be seen in some
patients even with successful denervation of the treated muscles. Clinicians may begin
treatment with a dose of 10.0 MU of Botox into each corrugator muscle, and may select
candidates for injection by determining the type of wrinkle to be treated and its spreadability
(glabellar spread test).
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37.) Botulinum A neurotoxin for axillary hyperhidrosis. No sweat Botox.
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Author
Glogau RG
Address
Department of Dermatology, University of California, San Francisco, USA.
Source
Dermatol Surg, 24(8):817-9 1998 Aug
Abstract
BACKGROUND: Axillary hyperhidrosis causes considerable emotional stress and is
associated with extraordinary costs and limitations in clothing. Existing topical and surgical
therapies are either ineffective or associated with unacceptable morbidity and sequelae.
Botulinum A neurotoxin (Botox) has been shown to decrease sweating in normal skin and in
palmar hyperhidrosis. OBJECTIVE: The current study was undertaken to demonstrate the
utility of using Botox in the treatment of axillary hyperhidrosis. METHODS: Twelve patient
with axillary hyperhidrosis underwent intradermal injection with 50 units of Botox in the
axillary skin bilaterally. RESULTS: All patients enjoyed relatively complete anhidrosis of the
axillary skin in periods ranging from 4 to 7 months. Repeat injections produced similar results.
CONCLUSION: Botulinum A neurotoxin (Botox) is an elegant and simple treatment for
axillary hyperhidrosis.
Language
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38.) Botox-induced prostatic involution.
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Author
Doggweiler R; Zermann DH; Ishigooka M; Schmidt RA
Address
Division of Urology, University of Colorado Health Science Center, Denver 80262, USA.
ragi.doggweiler@UCHSC.edu
Source
Prostate, 37(1):44-50 1998 Sep 15
Abstract
BACKGROUND: A simple approach to induced prostatic atrophy was explored. Surgical
denervation is known to produce profound atrophy of the rat prostate. Because Botulinum
toxin type A (Botox) produces a long-term chemical denervation, the potential to induce
atrophy of the rat prostate was explored. METHODS: Thirty rat prostates were injected with
varying doses of Botox. Single and serial injections were used, and rats were subsequently
sacrificed after either 1 or 4 weeks, respectively. The prostate glands were harvested,
weighed, and histologically studied for morphologic and apoptotic changes. RESULTS: The
total prostate volume and weight were found to be reduced in all Botox-injected animals.
Histologically, a generalized atrophy of the glands was observed with the H&E stain. There
was also diffuse glandular apoptosis evident with the Tunel stain. There were no significant
complications (e.g., urinary retention, weight loss, or hind/limb weakness).
CONCLUSIONS: Botulinum toxin type A injection into the prostate gland induces selective
denervation and subsequent atrophy of the prostate. Apoptosis was seen diffusely throughout
the gland. It may be possible that in the future, this long-acting neurotoxin could be used for
the treatment of common pathologies of the human prostate.
Language
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39.) Use of botulinum A toxin in patients at risk of wound complications following eyelid reconstruction.
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Author
Choi JC; Lucarelli MJ; Shore JW
Address
Ophthalmic Consultants of Boston, Massachusetts, USA.
Source
Ophthal Plast Reconstr Surg, 13(4):259-64 1997 Dec
Abstract
Our purpose was to determine the efficacy of botulinum A toxin (BOTOX) in promoting
wound immobilization and preventing wound dehiscence in patients at risk of wound-healing
complications following eyelid reconstruction. In 11 patients at risk of postoperative wound
complications, we injected BOTOX into the periocular musculature in addition to standard
suture tarsorrhaphy. Each patient experienced excellent wound immobilization and wound
healing. There were no complications. Adjuvant use of BOTOX, in conjunction with suture
tarsorrhaphy, immobilizes the eyelids and promotes wound healing in patients at risk of
wound complications following eyelid reconstruction.
Language
Eng
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40.) Cosmetic upper-facial rejuvenation with botulinum.
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Author
Ellis DA; Tan AK
Address
Department of Otolaryngology, University of Toronto, Ontario.
Source
J Otolaryngol, 26(2):92-6 1997 Apr
Abstract
OBJECTIVE: This study was conducted to evaluate the cosmetic use of botulinum toxin type
A (Botox), which blocks the release of acetylcholine at the presynaptic neuromuscular
junction leading to an irreversible, but temporary chemical denervation muscular paralysis and
weakness. This produces a significant cosmetic improvement of wrinkling in the upper face
due to hyperfunctional animation. METHOD: A prospective clinical study representing our
experience with this new technique is presented. Patient selection and evaluation,
classification of animation lines, techniques, results and complications are discussed. In a
15-month period, 23 patients with seven anatomic sites were injected. Twenty-three patients
had the lateral aspect and the inferior aspect of their squint lines injected, and 26 patients had
their glabellar frownlines injected. RESULTS: Significant improvement occurred to the
average depth and length of the glabellar frownlines. The subjective improvement by the
patients was also significant. Regarding the crow's feet, the lateral canthal lines showed more
improvement than the inferior lateral canthal lines because the latter has a greater component
of zygomaticus major and minor muscle, which contributes to the inferior lateral squint line.
CONCLUSION: Botox is a safe, easy-to-use, effective modality for the temporary elimination of hyperfunctioning upper-facial muscles.
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41.) New Treatment For Sweaty Palms Works for Up To A Year
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SCHAUMBURG, IL -- February 13, 1998 -- People who find no relief from
conventional drug treatment for the persistent problem of sweaty palms may get long-term improvement from injections of a potent bacterial toxin, according to a study reported in this month’s issue of the Journal of the American Academy of Dermatology.
Botulinum toxin type A is a powerful chemical that in its diluted prescription form (Botox) has been used safely in treating eye muscle disorders, wrinkles and other conditions. It reduces sweating by blocking release of the chemical
acetylcholine, which stimulates secretion of the sweat glands.
"Botulinum toxin safely and effectively inhibits excessive sweat production in the palms for as long as 12 months," said Walter Shelley, MD, PhD, a study co-author and dermatologist at the Medical College of Ohio, Toledo.
Earlier studies of botulinum toxin therapy for sweaty palms showed it reduced sweating for up to only three months.
Four months was the shortest improvement seen in the study conducted by
Shelley, Nickolai Talanin, MD, PhD, and E. Dorinda Shelley, MD. All patients experienced substantial improvement of their condition after receiving multiple injections of botulinum toxin. The drug was injected close to the sweat glands in the patients' palms after their skin was numbed with an anesthetic.
"These results offer good news to patients whose severe palm sweating is
resistant to other treatments and who want to avoid surgery," Shelley said.
Persistent sweating of the palms, called palmar hyperhidrosis, is caused by an abnormal sensitivity to acetylcholine.
"Palmar hyperhidrosis is not common," Shelley said. "However, individuals with severe cases often suffer social, psychological and occupational problems because of their disease."
Endoscopic surgery of the sympathetic nervous system, which controls
sweating, provides a permanent solution but requires general anesthesia andcan cause circulatory problems later.
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DATA-MEDICOS/DERMAGIC-EXPRESS No (21) 04/12/98 DR. JOSE LAPENTA R. DERMATOLOGO
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Produced by Dr. José Lapenta R. Dermatologist
Venezuela
1.998-2.024
Producido por Dr. José Lapenta R. Dermatólogo Venezuela 1.998-2.0024
Tlf: 0414-2976087 - 04127766810