Botulinum Toxin in the Field of Dermatology: Novel Indications
Abstract
:1. Introduction
2. Off-Label Use of BTX in Dermatology
2.1. BTX in Hypertrophic Scar Treatment
2.2. BTX in Scar Prevention
2.3. BTX in Rosacea and Facial Flushing
2.4. BTX in Postherpetic Neuralgia
2.5. BTX in Pruritus
2.6. BTX in Dermatological Conditions Associated with Hyperhidrosis
2.7. BTX in Oily Skin
3. Conclusions
Acknowledgments
Conflicts of Interest
References
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First Author [Ref.], Year | Type of Study | n | Treatment Regimen | Outcome Measures | Follow-Up | Results (Including Adverse Effects) |
---|---|---|---|---|---|---|
Elhefnawy [4], 2016 | Prospective, single arm (BTX) | 20 | BTX once a month for 3 months. BTX concentration: 5 IU/0.1 mL; Injected dose: 2.5 IU/cm3, not exceeding 100 IU/session | Overall assessment made by the patient and physician (5-point scale). Lesions were assessed for erythema, itching, and pliability; each item was assessed on a 5-point scale | 6 months | Therapeutic satisfaction was “good” in 14 patients, “excellent” in 6; The mean erythema score decreased from 3.2 to 1.0, mean pliability score from 3.3 to 0.8 and the mean itching score from 2.7 to 0.7; All findings were statistically significant. No recurrence or complications. |
Shaarawy [5], 2015 | Randomized, double-blinded, comparative study (BTX vs. IL steroid injection) | 24 | Group A (12 patients; Triamcinolone, Kenacort® 10 mg/cc; repeated every 4 weeks for 6 sessions/or till complete remission) Group B (12 patients; BTX 5 IU/cm3 repeated every 8 weeks for three sessions/or till complete remission of keloid) | Objective parameters (hardness, elevation, and redness) and subjective complaints (itching, pain and tenderness) on a scale of 0–3; Volume of keloid; Patient satisfaction (3-point scale) | 7 months | Significant decrease in scar volume after treatment with a volume reduction of 82.7% (group A) and 79.2% (group B). Significant softening, significant decrease in height and significant decrease in redness with little difference between the groups. All patients mentioned a significant reduction of their subjective complaints which was more prominent in group B (BTX group). Skin atrophy and telangiectasia was evident in 3 patients of group A. |
Xiao [6], 2009 | Prospective, single arm (BTX) | 19 | BTX once a month for a total of 3 months. BTX injection dose: 2.5 IU/cm3, not exceeding 100 IU/session. | Physician and patient satisfaction (5-point scale); Clinical symptoms in terms of erythema, pliability and itching sensation (each graded on a 5-point scale) | 6 months | Patient satisfaction: good (63.1%), excellent (36.8%) Physician satisfaction: good (78.9%), excellent (10.5%) Mean erythema score decreased from 3.41 to 1.23; The pliability score decreased from 3.85 to 0.78; and the itching score decreased from 3.50 to 0.83. All reductions were statistically significant. Besides the injection pain, no other complication was detected in this study. |
Zhibo [7], 2009 | Prospective, single arm (BTX) | 12 | BTX at 3 months interval for a maximum of 9 months. BTX concentration: 35 IU/mL; injected dose: 70–140 IU/session | Improvement was judged based on a decrease in size and flattening of the lesion with a 5-point scale; Patient satisfaction | 1 year | Therapeutic outcome: excellent (25%), good (41.7%), fair (33.3%). The level of patient satisfaction was very high. There were no serious adverse sequelae. |
First Author [Ref.], Year | Type of Study | n | Treatment Regimen | Outcome Measures | Follow-Up | Results (Including Adverse Effects) |
---|---|---|---|---|---|---|
Kim [19], 2014 | A split-scar, double-blind, RCT (BTX vs. saline) | 15 | Treatment with either BTX or 0.9% normal saline on scar halves. A single treatment delivered within 10 days of thyroidectomy. BTX concentration: 5 IU/mL; Injection dose: 20–65 IU | Modified Stony Brook Scar Evaluation Scale (SBSES) Patient satisfaction (4-point scale) | 6 months | A significant improvement in SBSES score was noted for the BTX-treated halves (p < 0.001), with minimal change on the saline-treated side. The mean calculated difference in SBSES scores (final/initial) between the BTX-treated side and the saline-treated side was also significant (p < 0.001). Subjects were significantly more satisfied with the overall outcome of the BTX-treated side at 6 months’ follow-up, according to a four-point grading scale (p = 0.000; 95% CI 1.24 to 2.36) |
Ziade [20], 2013 | RCT (BTX vs. no injection) | BTX group: 15 (4 lost for FU) Control group: 15 (2 lost for FU) | BTX group: A single treatment delivered within 72 h following op. BTX concentration: 10 IU/mL; Injection dose: 15–40 IU. Control group: No injection | Patient Scar Assessment Scale (PSAS) Observer Scar Assessment Scale (OSAS) Vancouver Scar Scale (VSS), Visual Analogue Scale (VAS) | 12 months | No statistically significant differences were found between the two groups for the PSAS, OSAS and VSS scores. The median VAS rated by the six evaluators was 8.25 for the botulinum toxin-treated group compared with 6.35 for the control group (p < 0.001). |
Gassner [21], 2006 | RCT (BTX vs. saline) | BTX group: 22 (6 excluded) Control group: 20 (5 excluded) | BTX group: A single injection within 24 h after wound closure. BTX concentration: 75 IU/mL; Injection dose: 15–45 IU. Control group: A single injection within 24 h after wound closure. Injection dose: 0.2–0.6 mL of saline | Visual Analogue Scale (VAS) | 6 months | The overall median VAS score for the BTX-treated group was 8.9 compared with 7.2 for the placebo group (p = 0.003), indicating enhanced healing and improved cosmesis of the experimentally immobilized scars. |
Wilson [22], 2006 | Prospective, single-arm | 55 (15 dropped out) | BTX was injected once at the end of the operation. BTX concentration: 10 IU/mL; Injection dose: 1.5 IU per cm of wound length. | Objective assessment Subjective assessment | 12–16 months | The outcome was considered highly satisfactory in 36 patients (90%). Thirty patients rated the improvement as marked (75%), six rated it as significant (15%), and four rated it as unchanged (10%). In 3 cases (7.5%), the scars re-widened, while in one case (2.5%), residual scar depression persisted. |
First Author [Ref.], Year | Type of Study | n | Treatment Regimen | Outcome Measures | Follow-Up | Results (Including Adverse Effects) |
---|---|---|---|---|---|---|
Eshghi [23], 2016 | Prospective single arm (BTX) | 24 | A single treatment with BTX. 1 IU of BTX was injected intracutaneously in every square cm, to a total dose of 30 IU on both sides of cheeks. | The Dermatology Life Quality Index (DLQI) | 2 months | The mean of DLQI improved from 8.08 ± 1.17 (baseline) to 4.5 ± 1.21 (2 months follow-up) (p < 0.005) |
Bloom [24], 2015 | Prospective, single arm (Abo-BTX) | 25 (15 completed the study) | A single treatment with abo-BTX. Abo-BTX concentration: 100 IU/mL; Injected dose: 15–45 IU to the nose, cheeks, forehead, and chin | Facial erythema assessed by a non-treating physician using a standardized grading system (0–3) | 3 months | The treatment resulted in statistically significant improvement in erythema grade at 1 (p < 0.05), 2 (p < 0.001), and 3 months (p < 0.05) after treatment when compared with baseline. |
Geddoa [25], 2013 | Prospective, single arm (BTX) | 22 (18 included in the final analysis) | A single treatment with BTX for 20 patients and two sessions of treatment for 2. BTX concentration: 10 IU/mL; Injected dose: 1–2 IU/cm2 with maximum total dose of 100 IU (neck and/or chest) | Dermatology Life Quality Index (DLQI) | 4 weeks | The mean change in DLQI (before-after treatment) was 3.56 ± 4.6, suggesting a significant improvement in quality of life at 4 weeks following treatment (p < 0.004) |
Odo [26], 2011 | RCT (Abo-BTX vs. saline) | 60 women with menopausal hot flushes Group BTX: 30 (25 completed) Group Control: 30 (23 completed) | A single treatment with either abo-BTX or saline. Group BTX: Abo-BTX concentration: 500 IU/3.2 mL; Injected dose: 6.2 IU at each selected point in the skin (40 injection points to the face, chest, neck, and scalp) Group Control: saline solution injected at a volume of 0.04 mL per injection point | Intensity of sweating, number of hot flashes, and Starch-Iodine test. Number of women reporting episodes of night sweating and mood changes | 6 months | The sweating and hot flashes were less severe than before abo-BTX treatment, especially at 2 months follow-up; In the control group, there was no significant difference in mean intensity of sweating or in the mean number of hot flashes. Other menopausal symptoms such as night sweats were found better 2 months after abo-BTX treatment than in the control group (p < 0.001). |
First Author [Ref.], Year | Type of Study | n | Treatment Regimen | Outcome Measures | Follow-Up | Results (Including Adverse Effects) |
---|---|---|---|---|---|---|
Ding [31], 2017 | Prospective, single arm (BTX) | 58 | A single session of treatment was performed. BTX concentration: 4 IU/mL; Injection dose: 50–100 IU in total | Pain severity (VAS) Neuropathy pain scale (NPS) Quality of Life Scale (SF-36) PHN seizure severity, seizure duration, and frequency of attacks. The use of painkillers | 6 months | At 6 months follow-up, a significant decrease in seizure frequency, seizure duration, VAS score, NPS score, SF-36 score and the required amount of painkiller was observed (p < 0.05). After BTX injection, 4 patients complained of pain around the injection area which disappeared within a week. |
Apalla [32], 2013 | Double-blinded RCT (BTX vs. saline) | BTX group: 15 Control group: 15 | BTX group: A single treatment delivered. BTX concentration: 25 IU/mL; Injection dose: each patient received 40 injections in total (5 IU/point). Control group: A single treatment with saline. | Pain severity (VA) Quality of sleep | 4 months | Thirteen patients from the experimental arm achieved at least 50% reduction in VAS score, compared with none of the placebo group (p < 0.001). BTX patients showed significant reduction in VAS pain scores between baseline and week 2, which persisted for a median period of 16 weeks. BTX patients showed significant reduction in sleep scores between baseline and week 2, which remained unchanged until week 16 (p < 0.001). Treatment was well-tolerated. |
Xiao [33], 2010 | Double-blinded RCT (BTX vs. 0.5% lidocaine vs. saline) | BTX group: 20 (19 completed) Lidocaine group: 20 (19 completed) Control group: 20 (18 completed) | BTX group: A single injection. BTX concentration: 5 IU/mL; Injection dose: 200 IU at maximum. Lidocaine group: A single session of treatment of the same volume as BTX. Control group: A single injection of the same volume as BTX | Visual Analogue Scale (VAS) Quality of Life Percent of Opioid use | 3 months | Compared with pretreatment, VAS pain scores decreased at day 7 and 3 months posttreatment in all 3 groups. However, the VAS pain scores of the BTX group decreased more significantly compared with lidocaine and placebo groups at day 7 and 3 months posttreatment (p < 0.01). Sleep time improved in all 3 groups but was most significant in the BTX group compared with the lidocaine and placebo groups (p < 0.01). The percentage of subjects using opioids posttreatment in the BTX was the lowest (21.1%), compared with the lidocaine (52.6%) and placebo (66.7%) groups (p < 0.01). |
First Author [Ref.], Year | Type of Study | n | Treatment Regimen | Outcome Measures | Follow-Up | Results (Including Adverse Effects) |
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Akhtar [38], 2012 | Prospective, single arm (BTX) | 9 | Treatment with BTX once on the burn scar. BTX concentration: 10–25 IU/mL; Injection dose: not stated | Severity of itch (0–10 scale) | 11.3 months on average | On average, the burn covered 24% of the total body surface area and 87.5% of patients rated their burn itch as being severe (>7 on the itch scale). Following the administration of BTX, this fell to 0 out of 10 in 4 weeks. The average duration of symptom free period was 9 months (3–18 months). |
Gazerani [39], 2009 | Double-blind, split arm, RCT (BTX vs. saline) | 14 | BTX treated arm: 5 IU of BTX was injected into the skin once. Control arm: The same volume of 0.9% saline as in the BTX treated side was injected. After BTX and saline injection, a skin prick test with histamine was performed on both sites. | Itch ratings (0–10 scale), itch area, neurogenic inflammation (visible flare area) Blood flow (Laser Doppler imaging) Cutaneous temperature (Infrared thermography | 1 week | BTX reduced the histamine-induced itch intensity (p < 0.001), and itch area (p = 0.011) compared with saline at all time points after treatment. The duration of itch was also shorter for BTX treated areas (p < 0.001), with a peak effect at day 7. The flare area was smaller in the BTX treated arm compared with the saline treated arm at all time points after treatment (p = 0.002). Findings from blood flow (p < 0.001), and temperature measurements (p < 0.001), clearly showed suppressive effects of BTX on vasomotor reactions, with the maximal effect on day 3 and 7. |
Heckmann [40], 2002 | Prospective, single arm (Abo-BTX) | 4 | Abo-BTX was injected to a total of 6 lichen simplex chronicus (LSC) patches once. Abo-BTX concentration: 100 IU/mL; Injection dose: 20–80 IU. | Sensation of pruritus (VAS 0–10) | 4 months | After a week, all patients reported a noticeable alleviation of itching. Three patients felt no more itching at all; in one patient pruritus was reduced to less than 50% according to the VAS used before and after treatment. After 4 weeks, 5 of 6 lesions had cleared without any other treatment. After 12 weeks, 3 patients were still free of symptoms. One patient who had one lesion on the shin developed a new lesion on the dorsum of his foot which was cleared in 2 weeks after BTX treatment. |
First Author [Ref.], Year | Type of Study | n | Treatment Regimen | Outcome Measures | Follow-Up | Results (Including Adverse Effects) |
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Pompholyx | ||||||
Swartling [52], 2002 | A side-by-side prospective controlled trial (BTX vs. no treatment) | 10 | BTX group: BTX was injected once. BTX concentration: 100 IU/mL; Injection dose: a mean of 162 IU. Control group: No treatment. | Effect of treatment (5-point scale) VAS for itch Disease activity score Extent of the dermatitis | 5–6 weeks | In the self-assessment, 7 of the 10 patients in the study experienced good or very good effect of the treatment. After injection with BTX, the VAS score for itching decreased by 39% on the treated side compared to an increase by 52% on the untreated side. Comparing treated vs. untreated sides, it was found that with BTX injection, a decrease in the disease activity score (54% vs. 29%), occurrence of vesicles (74 vs. 27), infiltration (54 vs. 18), erythema (53 vs. 30), and extent of the disease (58 vs. 31). No changes or only minor changes were seen in the objective parameters of scaling, crusting, and excoriations. |
Wollina [53], 2002 | A side-by-side prospective controlled trial (BTX vs. control) | 8 (6 completed the study) | Topical steroid was applied to both hands in combination with BTX on one hand and no additional treatment on the other. A single injection of BTX was given. BTX concentration: 50 IU/mL; BTX was injection in aliquots of 5 IU per point; Injection dose: Not mentioned. | Dyshidrotic Eczema Area and Severity Index (DASI) | 8 weeks | Six patients completed the study. The mean DASI score changed from 28 to 17 with topical therapy alone and from 36 to 3 with adjuvant BTX (p < 0.01). Itching and vesicles were inhibited earlier when using the combination of steroids and BTX. There was one relapse in the steroid group and none in the BTX group. |
Hidradenitis suppurativa | ||||||
Khoo [57], 2014 | Case report (BTX) | 3 (only one described in detail) | Over the course of 3 years, a Hurley Stage II HS patient received 4 BTX treatments. 50 IU of BTX administered to each axilla per treatment. BTX concentration: 25 IU/mL | The patient showed good clinical response within 3 months of her first treatment, and, following her second treatment, went into clinical remission. She was still in remission when discharged from follow-up 1 year after her fourth treatment. | ||
O’Reilly [56], 2005 | Case report (Abo-BTX) | 1 | BTX was injected once to both axilla. Injection dose: 250 IU of abo-BTX in total. | There was no evidence of active inflammation on follow-up at a fortnight after administration. The patient had complete remission of symptoms until approximately 10 months later, when the first symptoms of mild inflammation re-appeared. | ||
Psoriasis | ||||||
Zanchi [49], 2008 | Prospective, single-arm (BTX) | 15 | BTX was injected once to the inverse psoriasis sites. BTX concentration: 20 IU/mL; Dose injected: 50–100 IU in total. | Photographic assessment of the psoriatic area Subjective symptomatology (10-point VAS) | 12 weeks | The location of the psoriasis was as follows: armpits (7 patients), sub-mammary sulcus (6), intergluteal folds (7), inguinal folds (5) and umbilicus (1). Subjective symptomatology according to the 10-point VAS scale improved in all patients. Mean VAS scores were 9.1 at the pre-treatment assessment, with post-treatment mean scores of 4.2 after 2 weeks, 2.1 after 4 weeks and 2.4 after 12 weeks. Erythema extension, intensity and infiltration improved in 13 of 15 patients (87%). The change in the erythematous area was evident from the first post-treatment assessment at 2 weeks and continued to improve until the assessment at 4 weeks. At the final visit (12 weeks post-treatment), improvement had been maintained. |
Hailey–Hailey disease | ||||||
Lopez-Ferrer [60], 2012 | Case report (BTX) | 3 | Case 1: 80 IU of BTX was first administered on each axilla. A total of 200 IU of BTX was injected every 2 months for maintenance. Case 2: 80–300 IU of BTX was injected to the groin, below the left breast, the left axilla, and the side of the neck. Case 3: 200–300 IU of BTX was injected to the axilla, sub-mammary region, and groin. | The Hailey–Hailey disease improved in all 3 patients after BTX injection. BTX injection had to be repeated for maintaining remission. | ||
Konrad [61], 2001 | Case report with side-by side comparison (BTX alone vs. BTX + Erbium: YAG vs. BTX + dermabrasion | 1 | Both sub-mammary areas were treated with BTX at a concentration of 20 IU/mL. Four days later, surgical (right side) or laser therapy (left side) was performed on an area of 5 × 5 cm2. | Wound healing was faster after laser (7 days) versus dermabrasion (14 days). Those areas treated only with BTX showed remission of hyperhidrosis within 3 days and clearance of Hailey-Hailey within 2 weeks. During a follow-up of 12 months, no relapse was seen for dermabrasion, laser ablation and BTX. Final cosmetic results were comparable. |
First Author [Ref.], Year | Type of Study | n | Treatment Regimen | Outcome Measures | Follow-Up | Results (Including Adverse Effects) |
---|---|---|---|---|---|---|
Min [62], 2015 | Prospective (BTX 10 IU vs. BTX 20 IU) | 42 (41 completed the study) 20 received 10 IU of BTX 20 received 20 IU | Treatment with BTX once on the forehead. BTX concentration: 40 IU/mL; Injection dose: A final volume of 10 IU or 20 IU was injected evenly in 5 injection sites. | Sebum production (sebumeter) | 16 weeks | Treatment with BTX exhibited significant sebum alteration at the injection site of both groups (10 IU, 20 IU), with a sebum gradient surrounding the injection point. The efficacy did not improve at higher injection doses, with the four-unit regimen generally not being more potent than the two-unit regimen. The sebum production recovered to normal levels at the 16-week follow-up for both treatment groups, indicating that a higher dosage (4 units) did not results in a longer duration until relapse compared with the two-unit dose. |
Rose [63], 2012 | Prospective, single-arm (Abo-BTX) | 25 | Abo-BTX was injected once on the forehead. Abo-BTX concentration: 100 IU/mL; Injection dose: A total of 30–45 IU delivered to 10 injection sites. | Sebum production (sebumeter) Patient satisfaction (4-point scale) | 3 months | Treatment with BTX resulted in significantly lower sebum production at 1 week and 1, 2, and 3 months after injection (p < 0.001). Twenty-one patients (91%) reported that they were satisfied (50–75% improvement) with intradermal BTX as a treatment for oily skin. |
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Kim, Y.S.; Hong, E.S.; Kim, H.S. Botulinum Toxin in the Field of Dermatology: Novel Indications. Toxins 2017, 9, 403. https://doi.org/10.3390/toxins9120403
Kim YS, Hong ES, Kim HS. Botulinum Toxin in the Field of Dermatology: Novel Indications. Toxins. 2017; 9(12):403. https://doi.org/10.3390/toxins9120403
Chicago/Turabian StyleKim, Yoon Seob, Eun Sun Hong, and Hei Sung Kim. 2017. "Botulinum Toxin in the Field of Dermatology: Novel Indications" Toxins 9, no. 12: 403. https://doi.org/10.3390/toxins9120403
APA StyleKim, Y. S., Hong, E. S., & Kim, H. S. (2017). Botulinum Toxin in the Field of Dermatology: Novel Indications. Toxins, 9(12), 403. https://doi.org/10.3390/toxins9120403