fibrin and Histiocytoma--Benign-Fibrous

fibrin has been researched along with Histiocytoma--Benign-Fibrous* in 1 studies

Other Studies

1 other study(ies) available for fibrin and Histiocytoma--Benign-Fibrous

ArticleYear
Coagulation Factor XIII-A Subunit Missense Mutation in the Pathobiology of Autosomal Dominant Multiple Dermatofibromas.
    The Journal of investigative dermatology, 2020, Volume: 140, Issue:3

    Dermatofibromas are common benign skin lesions, the etiology of which is poorly understood. We identified two unrelated pedigrees in which there was autosomal dominant transmission of multiple dermatofibromas. Whole exome sequencing revealed a rare shared heterozygous missense variant in the F13A1 gene encoding factor XIII subunit A (FXIII-A), a transglutaminase involved in hemostasis, wound healing, tumor growth, and apoptosis. The variant (p.Lys679Met) has an allele frequency of 0.0002 and is predicted to be a damaging mutation. Recombinant human Lys679Met FXIII-A demonstrated reduced fibrin crosslinking activity in vitro. Of note, the treatment of fibroblasts with media containing Lys679Met FXIII-A led to enhanced adhesion, proliferation, and type I collagen synthesis. Immunostaining revealed co-localization between FXIII-A and α4β1 integrins, more prominently for Lys679Met FXIII-A than the wild type. In addition, both the α4β1 inhibitors and the mutation of the FXIII-A Isoleucine-Leucine-Aspartate-Threonine (ILDT) motif prevented Lys679Met FXIII-A-dependent proliferation and collagen synthesis of fibroblasts. Our data suggest that the Lys679Met mutation may lead to a conformational change in the FXIII-A protein that enhances α4-integrin binding and provides insight into an unexpected role for FXIII-A in the pathobiology of familial dermatofibroma.

    Topics: Catalytic Domain; Cell Proliferation; Collagen Type I; DNA Mutational Analysis; Exome Sequencing; Factor XIII; Female; Fibrin; Fibroblasts; HEK293 Cells; Histiocytoma, Benign Fibrous; Humans; Inheritance Patterns; Integrin alpha4; Male; Mutagenesis, Site-Directed; Mutation, Missense; Pedigree; Protein Conformation, alpha-Helical; Protein Conformation, beta-Strand; Recombinant Proteins; Skin; Structure-Activity Relationship

2020