Safety and early efficacy outcomes for lentiviral fibroblast gene therapy in recessive dystrophic epidermolysis bullosa

Lwin, Su M.; Syed, Farhatullah; Di, Wei; Kadiyirire, Tendai; Liu, Lu; Guy, Alyson; Petrova, Anastasia; Abdul‐Wahab, Alya; Reid, Fiona; Phillips, Robert; Elstad, Maria; Georgiadis, Christos; Aristodemou, Sophia; Lovell, Patricia A.; McMillan, James R.; Mee, John; Miskinyte, S.; Titeux, Matthias; Ozoemena, Linda; Pramanik, Rashida; Serrano, Sonia Simón; Rowles, Racheal; Maurin, Clarisse; Orrin, Elizabeth; Martinez-Queipo, Magdalena; Rashidghamat, Ellie; Tziotzios, Christos; Onoufriadis, Alexandros; Chen, Mei; Chan, Lucas; Farzaneh, Farzin; Río, Marcela Del; Tolar, Jakub; Bauer, Johann; Larcher, Fernando; Antoniou, Michael; Hovnanian, Alain; Thrasher, Adrian J.; Mellerio, Jemima E.; Qasim, Waseem; McGrath, John A.

doi:10.1172/jci.insight.126243

Cited by 67 publications

(63 citation statements)

References 40 publications

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“…Gene therapies aim at replacing or correcting disease-causing gene mutations in ex vivo patient cells, including induced pluripotent stem cells (iPSCs) [97], fibroblasts [98,99], and keratinocytes with high growth potential, termed holoclones. Different strategies ranging from retroviral-mediated gene transfer to genome editing (e.g., TALENs and CRISP/CAS9 systems) [100,101,102,103,104,105] can be used for gene correction in patient cells.…”

Section: Dystrophic Ebmentioning

confidence: 99%

Epidermolysis Bullosa-Associated Squamous Cell Carcinoma: From Pathogenesis to Therapeutic Perspectives

Condorelli

Dellambra

Logli

et al. 2019

IJMS

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Epidermolysis bullosa (EB) is a heterogeneous group of inherited skin disorders determined by mutations in genes encoding for structural components of the cutaneous basement membrane zone. Disease hallmarks are skin fragility and unremitting blistering. The most disabling EB (sub)types show defective wound healing, fibrosis and inflammation at lesional skin. These features expose patients to serious disease complications, including the development of cutaneous squamous cell carcinomas (SCCs). Almost all subjects affected with the severe recessive dystrophic EB (RDEB) subtype suffer from early and extremely aggressive SCCs (RDEB-SCC), which represent the first cause of death in these patients. The genetic determinants of RDEB-SCC do not exhaustively explain its unique behavior as compared to low-risk, ultraviolet-induced SCCs in the general population. On the other hand, a growing body of evidence points to the key role of tumor microenvironment in initiation, progression and spreading of RDEB-SCC, as well as of other, less-investigated, EB-related SCCs (EB-SCCs). Here, we discuss the recent advances in understanding the complex series of molecular events (i.e., fibrotic, inflammatory, and immune processes) contributing to SCC development in EB patients, cross-compare tumor features in the different EB subtypes and report the most promising therapeutic approaches to counteract or delay EB-SCCs.

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Section: Dystrophic Ebmentioning

confidence: 99%

Epidermolysis Bullosa-Associated Squamous Cell Carcinoma: From Pathogenesis to Therapeutic Perspectives

Condorelli

Dellambra

Logli

et al. 2019

IJMS

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“…Lwin et al . reported a similar observation in one patient who had been treated with intradermal injections of gene‐modified autologous fibroblasts in a phase I trial and had positive enzyme‐linked immunosorbent assay (ELISA) and enzyme‐linked immunosorbent spot (ELISpot) but negative indirect immunofluorescence (IIF) and no autoimmune symptoms after treatment …”

Section: Characteristics Of Patients With Recessive Dystrophic Epidermentioning

confidence: 66%

EBGene trial: patient preselection outcomes for the European GENEGRAFT ex vivo phase I/II gene therapy trial for recessive dystrophic epidermolysis bullosa

et al. 2019

Self Cite

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“…While, stem cell treatment employing iPSCs for some tissues/diseases may have its challenges, enormous progress has been made, making this an exciting approach [154]. For RDEB clinical trials employing ex vivo retroviral transduction of patient keratinocytes or fibroblasts to induce collagen VII expression followed by grafting or fibroblast injection, respectively, has shown promise [145,155]. These represent mutation-independent approaches for BM collagens.…”

Section: Treatment Interventionmentioning

confidence: 99%

“…Mitochondrial dysfunction and dysregulation of autophagy resulting from collagen VI or XV/XVIII deficiency was ameliorated by dietary and pharmacological treatments when tested in mice and patient-derived cells [82,37,123,126], indicating a convergent mechanism and treatment. Re-instating collagen expression via cell graft or cell transplant represents a different approach and has shown promise for collagen VI and VII [81,145,155,129]. Re-instating Col6a1 expression also rescued the defective muscle stem cell renewal in Col6a1 −/− mice, which was recalcitrant to autophagy treatment [81], suggesting a combinatorial therapy may be required.…”

Section: Treatment Interventionmentioning

confidence: 99%

Basement membrane collagens and disease mechanisms

Gatseva

Sin

Brezzo

et al. 2019

Essays in Biochemistry

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Basement membranes (BMs) are specialised extracellular matrix (ECM) structures and collagens are a key component required for BM function. While collagen IV is the major BM collagen, collagens VI, VII, XV, XVII and XVIII are also present. Mutations in these collagens cause rare multi-systemic diseases but these collagens have also been associated with major common diseases including stroke. Developing treatments for these conditions will require a collective effort to increase our fundamental understanding of the biology of these collagens and the mechanisms by which mutations therein cause disease. Novel insights into pathomolecular disease mechanisms and cellular responses to these mutations has been exploited to develop proof-of-concept treatment strategies in animal models. Combined, these studies have also highlighted the complexity of the disease mechanisms and the need to obtain a more complete understanding of these mechanisms. The identification of pathomolecular mechanisms of collagen mutations shared between different disorders represent an attractive prospect for treatments that may be effective across phenotypically distinct disorders.

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Safety and early efficacy outcomes for lentiviral fibroblast gene therapy in recessive dystrophic epidermolysis bullosa

Cited by 67 publications

References 40 publications

Epidermolysis Bullosa-Associated Squamous Cell Carcinoma: From Pathogenesis to Therapeutic Perspectives

Epidermolysis Bullosa-Associated Squamous Cell Carcinoma: From Pathogenesis to Therapeutic Perspectives

EBGene trial: patient preselection outcomes for the European GENEGRAFT ex vivo phase I/II gene therapy trial for recessive dystrophic epidermolysis bullosa

Basement membrane collagens and disease mechanisms

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