Mutant GNLY is linked to Stevens–Johnson syndrome and toxic epidermal necrolysis

Autor:	Heidi Mateus, Dora Janeth Fonseca, Luz Adriana Caro, David Bolívar-Salazar, Ana Francisca Ramírez, Alejandra de-la-Torre, Yohjana Carolina Suárez, Diana Carolina Sierra-Diaz, Olga Londoño, Paul Laissue, Carlos Serrano-Reyes
Jazyk:	angličtina
Rok vydání:	2019
Předmět:	Antigens Differentiation T-Lymphocyte Contrast medium Male Keratinocytes Cellular distribution Sanger sequencing Apoptosis Pathogenesis Gene mutation Gene sequence Western blotting Computer model Mutant protein t-lymphocyte Pathology Granulysin Child Middle aged Genetics (clinical) Priority journal 0303 health sciences 030305 genetics & heredity Urtica dioica differentiation Gnly protein Middle Aged Pyrimethamine plus sulfadoxine Cocodamol Carbamazepine Child Preschool Female Animal cell Keratinocyte medicine.drug Human Phenytoin Adult Heterozygote Adolescent Metoclopramide Clinical article Stevens johnson syndrome Case control study Cho cell line Genetic predisposition to disease Case-control studies Biology Lamotrigine Sulfonamide Pathophysiology Article preschool 03 medical and health sciences Young Adult Necrosis GNLY Stevens-johnson syndrome medicine Genetic predisposition Genetics T lymphocyte antigen Humans Genetic Predisposition to Disease Antigens Codon 030304 developmental biology Protein localization Cefalexin Infant Toxic epidermal necrolysis medicine.disease Nonhuman Gene frequency Cotrimoxazole stomatognathic diseases Biological marker Young adult Metabolism Preschool child Case-Control Studies Stevens-Johnson Syndrome Immunology Mutation Mutant proteins Mutant Proteins School child Nucleotide sequence Biomarkers
Zdroj:	Repositorio EdocUR-U. Rosario Universidad del Rosario instacron:Universidad del Rosario
Popis:	Stevens–Johnson syndrome (SJS) and toxic epidermal necrolysis (TEN) are rare severe cutaneous adverse reactions to drugs. Granulysin (GNLY) plays a key role in keratinocyte apoptosis during SJS/TEN pathophysiology. To determine if GNLY-encoding mutations might be related to the protein’s functional disturbances, contributing to SJS/TEN pathogenesis, we performed direct sequencing of GNLY’s coding region in a group of 19 Colombian SJS/TEN patients. A GNLY genetic screening was implemented in a group of 249 healthy individuals. We identified the c.11G > A heterozygous sequence variant in a TEN case, which creates a premature termination codon (PTC) (p.Trp4Ter). We show that a mutant protein is synthesised, possibly due to a PTC-readthrough mechanism. Functional assays demonstrated that the mutant protein was abnormally located in the nuclear compartment, potentially leading to a toxic effect. Our results argue in favour of GNLY non-synonymous sequence variants contributing to SJS/TEN pathophysiology, thereby constituting a promising, clinically useful molecular biomarker. © 2019, Springer-Verlag GmbH Germany, part of Springer Nature.
Databáze:	OpenAIRE
Externí odkaz:	https://explore.openaire.eu/search/publication?articleId=doi_dedup___::80ab220339d0ba6ca40fd98285659b05 https://repository.urosario.edu.co/handle/10336/24215 Zobrazit plný text záznamu