Characterization of Novel Missense Variants of <i>SERPINA1</i> Gene Causing Alpha-1 Antitrypsin Deficiency

Nerea Matamala(Instituto de Investigación de Enfermedades Raras), Beatriz Lara(University Hospital Coventry), Gema Gómez‐Mariano(Instituto de Investigación de Enfermedades Raras), Selene Martínez(Instituto de Investigación de Enfermedades Raras), Diana Retana(Instituto de Investigación de Enfermedades Raras), T Fernandez(Instituto de Investigación de Enfermedades Raras), Ramona A. Silvestre(Hospital Universitario Puerta de Hierro Majadahonda), Irene Belmonte(Vall d'Hebron Hospital Universitari), Francisco Rodríguez‐Frias(Vall d'Hebron Hospital Universitari), Marçal Vilar(Consejo Superior de Investigaciones Científicas), Raquel Sáez González(Biogipuzkoa Health Research Institute), Igor Iturbe, Silvia Castillo(Hospital Clínico Universitario de Valencia), María Molina‐Molina(Bellvitge University Hospital), Anna Texidó(Hospital Universitari Sant Joan de Reus), Gema Tirado-Conde(Complejo Hospitalario Universitario de Granada), José Luís López-Campos(Centro de Investigación Biomédica en Red de Enfermedades Respiratorias), Manuel Posada de la Paz(Instituto de Salud Carlos III), Ignacio Blanco(Sociedad Española de Neumología y Cirugía Torácica), Sabina Janciauskiene(Medizinische Hochschule Hannover), Beatriz Martínez–Delgado(Instituto de Investigación de Enfermedades Raras)
American Journal of Respiratory Cell and Molecular Biology
December 12, 2017
10.1165/rcmb.2017-0179oc
Cited by 32Open Access
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Abstract

The SERPINA1 gene is highly polymorphic, with more than 100 variants described in databases. SERPINA1 encodes the alpha-1 antitrypsin (AAT) protein, and severe deficiency of AAT is a major contributor to pulmonary emphysema and liver diseases. In Spanish patients with AAT deficiency, we identified seven new variants of the SERPINA1 gene involving amino acid substitutions in different exons: PiSDonosti (S+Ser14Phe), PiTijarafe (Ile50Asn), PiSevilla (Ala58Asp), PiCadiz (Glu151Lys), PiTarragona (Phe227Cys), PiPuerto Real (Thr249Ala), and PiValencia (Lys328Glu). We examined the characteristics of these variants and the putative association with the disease. Mutant proteins were overexpressed in HEK293T cells, and AAT expression, polymerization, degradation, and secretion, as well as antielastase activity, were analyzed by periodic acid-Schiff staining, Western blotting, pulse-chase, and elastase inhibition assays. When overexpressed, S+S14F, I50N, A58D, F227C, and T249A variants formed intracellular polymers and did not secrete AAT protein. Both the E151K and K328E variants secreted AAT protein and did not form polymers, although K328E showed intracellular retention and reduced antielastase activity. We conclude that deficient variants may be more frequent than previously thought and that their discovery is possible only by the complete sequencing of the gene and subsequent functional characterization. Better knowledge of SERPINA1 variants would improve diagnosis and management of individuals with AAT deficiency.

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