Literature DB >> 32178539

Leading edge: emerging drug, cell, and gene therapies for junctional epidermolysis bullosa.

Allison R Keith1,2, Kirk Twaroski1,2, Christen L Ebens1, Jakub Tolar1,2.   

Abstract

INTRODUCTION: Junctional epidermolysis bullosa (JEB) is a rare inherited genetic disorder with limited treatments beyond palliative care. A major hallmark of JEB is skin blistering caused by functional loss or complete absence of major structural proteins of the skin. Impaired wound healing in patients with JEB gives rise to chronic cutaneous ulcers that require daily care. Wound care and infection control are the current standard of care for this patient population. AREAS COVERED: This review covers research and clinical implementation of emerging drug, cell, and gene therapies for JEB. Current clinical trials use topical drug delivery to manipulate the inflammation and re-epithelialization phases of wound healing or promote premature stop codon readthrough to accelerate chronic wound closure. Allogeneic cell therapies for JEB have been largely unsuccessful, with autologous skin grafting emerging as a reliable method of resolving the cutaneous manifestations of JEB. Genetic correction and transplant of autologous keratinocytes have demonstrated persistent amelioration of chronic wounds in a subset of patients. EXPERT OPINION: Emerging therapies address the cutaneous symptoms of JEB but are unable to attend to systemic manifestations of the disease. Investigations into the molecular mechanism(s) underpinning the failure of systemic allogeneic cell therapies are necessary to expand the range of effective JEB therapies.

Entities:  

Keywords:  Basement membrane zone; cell therapy; clinical trials; drug therapy; extracellular matrix; gene therapy; hematopoietic cell transplant; junctional epidermolysis bullosa; keratinocytes; wound healing

Mesh:

Substances:

Year:  2020        PMID: 32178539      PMCID: PMC7392816          DOI: 10.1080/14712598.2020.1740678

Source DB:  PubMed          Journal:  Expert Opin Biol Ther        ISSN: 1471-2598            Impact factor:   4.388


  109 in total

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5.  Immunogenicity of decidual stromal cells in an epidermolysis bullosa patient and in allogeneic hematopoietic stem cell transplantation patients.

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6.  Amelioration of epidermolysis bullosa by transfer of wild-type bone marrow cells.

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7.  In vitro and in vivo gene therapy vector evolution via multispecies interbreeding and retargeting of adeno-associated viruses.

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8.  Structural basis for the inhibition of the eukaryotic ribosome.

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Journal:  PLoS One       Date:  2014-01-22       Impact factor: 3.240

10.  High-fidelity CRISPR-Cas9 nucleases with no detectable genome-wide off-target effects.

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2.  Interrogation of RDEB Epidermal Allografts after BMT Reveals Coexpression of Collagen VII and Keratin 15 with Proinflammatory Immune Cells and Fibroblasts.

Authors:  Julia A Riedl; Megan Riddle; Lily Xia; Cindy Eide; Christina Boull; Christen L Ebens; Jakub Tolar
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3.  Modified Non-Cultured Cell Spray Induced Epithelization in LAMB3 Mutation Epidermolysis Bullosa.

Authors:  Suci Widhiati; Shinta Trilaksmi Dewi; Retno Danarti; Hardyanto Soebono; Yulia Eka Irmawati; Monika Puspitasari; Niken Trisnowati; Tri Wibawa; Dewajani Purnomosari; Yohanes Widodo Wirohadidjojo
Journal:  Clin Cosmet Investig Dermatol       Date:  2022-10-14

Review 4.  Junctional epithelium and hemidesmosomes: Tape and rivets for solving the "percutaneous device dilemma" in dental and other permanent implants.

Authors:  Nicholas G Fischer; Conrado Aparicio
Journal:  Bioact Mater       Date:  2022-03-19

Review 5.  Ex vivo gene modification therapy for genetic skin diseases-recent advances in gene modification technologies and delivery.

Authors:  Vignesh Jayarajan; Evangelia Kounatidou; Waseem Qasim; Wei-Li Di
Journal:  Exp Dermatol       Date:  2021-03-11       Impact factor: 3.960

6.  Translational perspectives to treat Epidermolysis bullosa-Where do we stand?

Authors:  Christine Prodinger; Johann W Bauer; Martin Laimer
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  6 in total

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