Effective and durable repigmentation for stable vitiligo: A randomized within-subject controlled trial assessing treatment with autologous skin cell suspension transplantation

Vitiligo lesions are often challenging to repigment with conventional medical therapies. Surgical autologous melanocyte transfer methods can be utilized for stable vitiligo but demand specialized skills and equipment. A point-of-care autologous cell harvesting device was designed enabling simple pre...

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Published in	Journal of the American Academy of Dermatology Vol. 91; no. 6; pp. 1104 - 1112
Main Authors	Hamzavi, Iltefat H., Ganesan, Anand K., Mahmoud, Bassel H., Weiss, Eduardo, Ahmed, Ammar M., Robinson, Deanne, Goldman, Mitchel P., Munavalli, Girish, Kahn, Steven A., Huang, Victor, Waibel, Jill, Desai, Alpesh, Elbuluk, Nada, Desai, Seemal, Pandya, Amit G.
Format	Journal Article
Language	English
Published	United States Elsevier Inc 01.12.2024
Subjects	Adult autologous cell transfer autologous skin cell suspension cellular grafting Female Fibroblasts - transplantation Humans Keratinocytes - transplantation Male melanocyte transfer Melanocytes - transplantation Middle Aged noncultured skin cell suspension procedural dermatology repigmentation Skin Pigmentation Skin Transplantation - methods Transplantation, Autologous Treatment Outcome Ultraviolet Therapy - methods vitiligo Vitiligo - therapy vitiligo surgery Young Adult autologous cell transfer autologous skin cell suspension cellular grafting FDA AE melanocyte transfer vitiligo procedural dermatology repigmentation CRC MKT noncultured skin cell suspension ASCS vitiligo surgery F-VASI US
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ISSN	0190-9622 1097-6787 1097-6787
DOI	10.1016/j.jaad.2024.08.027

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Abstract	Vitiligo lesions are often challenging to repigment with conventional medical therapies. Surgical autologous melanocyte transfer methods can be utilized for stable vitiligo but demand specialized skills and equipment. A point-of-care autologous cell harvesting device was designed enabling simple preparation of autologous skin cell suspension (ASCS) containing melanocytes, keratinocytes, and fibroblasts providing a straightforward approach for cellular transplantation. To evaluate the safety and effectiveness of ASCS for repigmentation of stable vitiligo lesions among adults. A US multicenter, randomized, within-subject controlled trial compared ASCS to narrow band ultraviolet B only (Control) in similar vitiligo lesions. ASCS was applied after laser skin resurfacing and followed by narrow band ultraviolet B treatment. The primary effectiveness endpoint was the proportion of lesions achieving ≥80% repigmentation at week-24. Repigmentation durability was assessed at week-52. Among 25 subjects, 36% of ASCS-treated lesions achieved ≥80% repigmentation at week-24 compared to 0% for Control (P < .025), with durability through week-52. The safety profile of ASCS was acceptable, with favorable patient- and investigator-reported outcomes. Study sample size limited robust subgroup analyses. Application of ASCS has potential as a treatment for repigmentation of stable vitiligo lesions with the potential to improve health-related quality of life and reduce burden of disease.
AbstractList	Vitiligo lesions are often challenging to repigment with conventional medical therapies. Surgical autologous melanocyte transfer methods can be utilized for stable vitiligo but demand specialized skills and equipment. A point-of-care autologous cell harvesting device was designed enabling simple preparation of autologous skin cell suspension (ASCS) containing melanocytes, keratinocytes, and fibroblasts providing a straightforward approach for cellular transplantation. To evaluate the safety and effectiveness of ASCS for repigmentation of stable vitiligo lesions among adults. A US multicenter, randomized, within-subject controlled trial compared ASCS to narrow band ultraviolet B only (Control) in similar vitiligo lesions. ASCS was applied after laser skin resurfacing and followed by narrow band ultraviolet B treatment. The primary effectiveness endpoint was the proportion of lesions achieving ≥80% repigmentation at week-24. Repigmentation durability was assessed at week-52. Among 25 subjects, 36% of ASCS-treated lesions achieved ≥80% repigmentation at week-24 compared to 0% for Control (P < .025), with durability through week-52. The safety profile of ASCS was acceptable, with favorable patient- and investigator-reported outcomes. Study sample size limited robust subgroup analyses. Application of ASCS has potential as a treatment for repigmentation of stable vitiligo lesions with the potential to improve health-related quality of life and reduce burden of disease. Vitiligo lesions are often challenging to repigment with conventional medical therapies. Surgical autologous melanocyte transfer methods can be utilized for stable vitiligo but demand specialized skills and equipment. A point-of-care autologous cell harvesting device was designed enabling simple preparation of autologous skin cell suspension (ASCS) containing melanocytes, keratinocytes, and fibroblasts providing a straightforward approach for cellular transplantation.BACKGROUNDVitiligo lesions are often challenging to repigment with conventional medical therapies. Surgical autologous melanocyte transfer methods can be utilized for stable vitiligo but demand specialized skills and equipment. A point-of-care autologous cell harvesting device was designed enabling simple preparation of autologous skin cell suspension (ASCS) containing melanocytes, keratinocytes, and fibroblasts providing a straightforward approach for cellular transplantation.To evaluate the safety and effectiveness of ASCS for repigmentation of stable vitiligo lesions among adults.OBJECTIVETo evaluate the safety and effectiveness of ASCS for repigmentation of stable vitiligo lesions among adults.A US multicenter, randomized, within-subject controlled trial compared ASCS to narrow band ultraviolet B only (Control) in similar vitiligo lesions. ASCS was applied after laser skin resurfacing and followed by narrow band ultraviolet B treatment. The primary effectiveness endpoint was the proportion of lesions achieving ≥80% repigmentation at week-24. Repigmentation durability was assessed at week-52.METHODSA US multicenter, randomized, within-subject controlled trial compared ASCS to narrow band ultraviolet B only (Control) in similar vitiligo lesions. ASCS was applied after laser skin resurfacing and followed by narrow band ultraviolet B treatment. The primary effectiveness endpoint was the proportion of lesions achieving ≥80% repigmentation at week-24. Repigmentation durability was assessed at week-52.Among 25 subjects, 36% of ASCS-treated lesions achieved ≥80% repigmentation at week-24 compared to 0% for Control (P < .025), with durability through week-52. The safety profile of ASCS was acceptable, with favorable patient- and investigator-reported outcomes.RESULTSAmong 25 subjects, 36% of ASCS-treated lesions achieved ≥80% repigmentation at week-24 compared to 0% for Control (P < .025), with durability through week-52. The safety profile of ASCS was acceptable, with favorable patient- and investigator-reported outcomes.Study sample size limited robust subgroup analyses.LIMITATIONSStudy sample size limited robust subgroup analyses.Application of ASCS has potential as a treatment for repigmentation of stable vitiligo lesions with the potential to improve health-related quality of life and reduce burden of disease.CONCLUSIONApplication of ASCS has potential as a treatment for repigmentation of stable vitiligo lesions with the potential to improve health-related quality of life and reduce burden of disease.
Author	Weiss, Eduardo Kahn, Steven A. Hamzavi, Iltefat H. Desai, Alpesh Robinson, Deanne Goldman, Mitchel P. Desai, Seemal Huang, Victor Elbuluk, Nada Munavalli, Girish Waibel, Jill Ahmed, Ammar M. Mahmoud, Bassel H. Pandya, Amit G. Ganesan, Anand K.
Author_xml	– sequence: 1 givenname: Iltefat H. orcidid: 0000-0002-3137-5601 surname: Hamzavi fullname: Hamzavi, Iltefat H. email: IHAMZAV1@hfhs.org organization: Department of Dermatology, Henry Ford Health System, Dermatology Research, Detroit, Michigan – sequence: 2 givenname: Anand K. surname: Ganesan fullname: Ganesan, Anand K. organization: Department of Dermatology, University of California Irvine, Irvine, California – sequence: 3 givenname: Bassel H. surname: Mahmoud fullname: Mahmoud, Bassel H. organization: Department of Dermatology, University of Massachusetts, Worcester, Massachusetts – sequence: 4 givenname: Eduardo surname: Weiss fullname: Weiss, Eduardo organization: Skin Care Research, Hollywood, Florida – sequence: 5 givenname: Ammar M. surname: Ahmed fullname: Ahmed, Ammar M. organization: Department of Internal Medicine, Dell Medical School at the University of Texas at Austin, Austin, Texas – sequence: 6 givenname: Deanne surname: Robinson fullname: Robinson, Deanne organization: DMR Research PLLC, Westport, Connecticut – sequence: 7 givenname: Mitchel P. surname: Goldman fullname: Goldman, Mitchel P. organization: Cosmetic Laser Dermatology: A Platinum Dermatology Partners Company, San Diego, California – sequence: 8 givenname: Girish surname: Munavalli fullname: Munavalli, Girish organization: Dermatology, Laser, & Vein Specialists of the Carolinas, Charlotte, North Carolina – sequence: 9 givenname: Steven A. surname: Kahn fullname: Kahn, Steven A. organization: Department of Surgery, Medical University of South Carolina, Charleston, South Carolina – sequence: 10 givenname: Victor surname: Huang fullname: Huang, Victor organization: Department of Dermatology, University of California, Sacramento, California – sequence: 11 givenname: Jill surname: Waibel fullname: Waibel, Jill organization: Miami Dermatology & Laser Research, Miami, Florida – sequence: 12 givenname: Alpesh surname: Desai fullname: Desai, Alpesh organization: Heights Dermatology & Aesthetic Center, Houston, Texas – sequence: 13 givenname: Nada surname: Elbuluk fullname: Elbuluk, Nada organization: Department of Dermatology, Keck School of Medicine USC, Los Angeles, California – sequence: 14 givenname: Seemal surname: Desai fullname: Desai, Seemal organization: Innovative Dermatology, Plano, Texas – sequence: 15 givenname: Amit G. surname: Pandya fullname: Pandya, Amit G. organization: Palo Alto Foundation Medical Group, Sunnyvale, California
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Keywords	autologous cell transfer autologous skin cell suspension cellular grafting FDA AE melanocyte transfer vitiligo procedural dermatology repigmentation CRC MKT noncultured skin cell suspension ASCS vitiligo surgery F-VASI US
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Snippet	Vitiligo lesions are often challenging to repigment with conventional medical therapies. Surgical autologous melanocyte transfer methods can be utilized for...
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SubjectTerms	Adult autologous cell transfer autologous skin cell suspension cellular grafting Female Fibroblasts - transplantation Humans Keratinocytes - transplantation Male melanocyte transfer Melanocytes - transplantation Middle Aged noncultured skin cell suspension procedural dermatology repigmentation Skin Pigmentation Skin Transplantation - methods Transplantation, Autologous Treatment Outcome Ultraviolet Therapy - methods vitiligo Vitiligo - therapy vitiligo surgery Young Adult
Title	Effective and durable repigmentation for stable vitiligo: A randomized within-subject controlled trial assessing treatment with autologous skin cell suspension transplantation
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