Small molecule drug development for rare genodermatoses – evaluation of the current status in epidermolysis bullosa

Wally, Verena; Reisenberger, Manuela; Kitzmüller, Sophie; Laimer, Martin

doi:10.1186/s13023-020-01467-9

Cited by 15 publications

(12 citation statements)

References 91 publications

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“…Over the past two decades, several treatment strategies for RDEB have been suggested and investigated (9)(10)(11)(12), yet cure or even effective symptom relief have not been achieved. Much research focuses on strategies targeting the genetic defect at the protein, mRNA or DNA level (12)(13)(14)(15).…”

Section: Introductionmentioning

confidence: 99%

Clinical trial of ABCB5+ mesenchymal stem cells for recessive dystrophic epidermolysis bullosa

Kiritsi¹,

Dieter²,

Niebergall-Roth³

et al. 2021

JCI Insight

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Background. Recessive dystrophic epidermolysis bullosa (RDEB) is a rare, devastating, and life-threatening inherited skin fragility disorder due to a lack of functional type VII collagen, for which no effective therapy exists. ABCB5-positive dermal mesenchymal stem cells (ABCB5 + MSCs) possess immunomodulatory, inflammation-dampening and tissue-healing capacities. In a Col7a1 -/mouse model of RDEB, treatment with ABCB5 + MSCs markedly extended the animals' lifespans.Methods. In this international, multicentric, single-arm, phase I/IIa clinical trial, 16 patients (aged 4-36 years) enrolled into four age cohorts received three intravenous infusions of 2×10 6 ABCB5 + MSCs/kg on days 0, 17 and 35. Patients were followed up for 12 weeks regarding efficacy and 12 months regarding safety. Results. At 12 weeks, statistically significant median (IQR) reductions in the EpidermolysisBullosa Disease Activity and Scarring Index activity (EBDASI activity) score of 13.0%(2.9%-30%; p=0.049) and the Instrument for Scoring Clinical Outcome of Research for Epidermolysis Bullosa clinician (iscorEB-c) score of 18.2% (1.9%-39.8%; p=0.037) were observed. Reductions in itch and pain numerical rating scale scores were greatest on day 35, amounting to 37.5% (0.0%-42.9%; p=0.033) and 25.0% (-8.4%-46.4%; p=0.168), respectively. Three adverse events were considered related to the cell product, one mild lymphadenopathy and two hypersensitivity reactions. The latter two were serious but resolved without sequelae shortly after withdrawal of treatment. Conclusion.This trial demonstrates good tolerability, manageable safety and potential efficacy of intravenous ABCB5 + MSCs as a readily available disease-modifying therapy for RDEB and provides a rationale for further clinical evaluation.

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Section: Introductionmentioning

confidence: 99%

Clinical trial of ABCB5+ mesenchymal stem cells for recessive dystrophic epidermolysis bullosa

Kiritsi¹,

Dieter²,

Niebergall-Roth³

et al. 2021

JCI Insight

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“…In the context of EB several approaches addressing various complications have been reported, with the majority of primary outcomes measured being improvement of wound healing, reduction of blistering, and mitigation of itch. While some of the evaluated compounds have reached late stage clinical trials, first marketing approvals are still awaited [4][5][6][7]69].…”

Section: Treating Complications Of Ebmentioning

confidence: 99%

“…While in some patients blisters heal without scarring, in patients suffering from more severe subtypes these degenerate into wounds and are accompanied by multiple comorbidities. Thus, preventing blistering or accelerating their resolution is a logical primary outcome measure for clinical trials due to its relevance to patients, at least in distinct patient cohorts [7]. Particularly in EBS, where patients only rarely develop wounds, reducing blister numbers will improve patients' QoL substantially.…”

Section: Reduction Of Blisteringmentioning

confidence: 99%

“…learning to walk, or playing with other children. However, also for dystrophic and junctional EB clinical studies evaluating a treatment's impact on blister numbers have been published [7].…”

Section: Reduction Of Blisteringmentioning

confidence: 99%

“…However, the increasing number of trials that are being conducted reflects significant progress in clinical research, including strategies to correct and/or modulate the aberrant molecules and mechanisms underlying this devastating disease. [4][5][6][7] The remarkable differences between EB-types and numerous subtypes, renders the development of therapies a complex challenge, as both inter-subtype and inter-individual differences require the development of more personalized treatments.…”

Section: Introductionmentioning

confidence: 99%

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Therapy Development for Epidermolysis Bullosa

Hofbauer¹,

Wally²,

Guttmann‐Gruber³

et al. 2021

Rare Diseases - Diagnostic and Therapeutic Odyssey

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Although rare genodermatoses such as Epidermolysis bullosa have received more attention over the last years, no approved treatment options targeting causal mutations are currently available. Still, such diseases can be devastating, in some cases even associated with life-threatening secondary manifestations. Therefore, developing treatments that target disease-associated complications along with causal therapies remains the focus of current research efforts, in order to increase patient’s quality of life and potentially their life expectancy. Epidermolysis bullosa is a genodermatosis that is caused by mutations in either one of 16 genes, predominantly encoding structural components of the skin and mucosal epithelia that are crucial to give these barrier organs physical and mechanical resilience to stress. The genetic heterogeneity of the disease is recapitulated in the high variability of phenotypic expressivity observed, ranging from minor and localized blistering to generalized erosions and wound chronification, rendering certain subtypes a systemic disease that is complicated by a plethora of secondary manifestations. During the last decades, several studies have focused on developing treatments for EB patients and significant progress has been made, as reflected by numerous publications, patents, and registered trials available. Overall, strategies range from causal to symptom-relieving approaches, and include gene, RNA and cell therapies, as well as drug developments based on biologics and small molecules. In this chapter, we highlight the most recent and promising approaches that are currently being investigated in order to provide effective treatments for patients with epidermolysis bullosa in the future.

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Genetic Blistering Diseases

McGrath

2024

Rook's Textbook of Dermatology

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The integrity of the skin is maintained by complex networks of structural and non‐structural proteins within the epidermis, epidermal basement membrane zone and upper dermis. Disruption to the function of any one of these integral proteins through inherited gene mutations can make the skin less resilient to trauma and more prone to blister formation. This chapter provides an overview of key proteins involved in skin integrity and outlines the spectrum of blistering diseases linked to abnormalities therein. The text also describes approaches to diagnosis of inherited blistering diseases, as well as innovative therapies which try to reduce blistering and improve skin function.

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Small molecule drug development for rare genodermatoses – evaluation of the current status in epidermolysis bullosa

Cited by 15 publications

References 91 publications

Clinical trial of ABCB5+ mesenchymal stem cells for recessive dystrophic epidermolysis bullosa

Clinical trial of ABCB5+ mesenchymal stem cells for recessive dystrophic epidermolysis bullosa

Therapy Development for Epidermolysis Bullosa

Genetic Blistering Diseases

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