Whole-Exome Sequencing, Proteome Landscape, and Immune Cell Migration Patterns in a Clinical Context of Menkes Disease

Author:

Martinez-Fierro Margarita L.ORCID,Cabral-Pacheco Griselda A.,Garza-Veloz IdaliaORCID,Acuña-Quiñones Jesus,Martinez-de-Villarreal Laura E.ORCID,Ibarra-Ramirez MarisolORCID,Beuten Joke,Sanchez-Guerrero Samantha E.,Villarreal-Martinez Laura,Delgado-Enciso IvanORCID,Rodriguez-Sanchez Iram P.,Zuñiga-Ramirez Vania Z.,Cardenas-Vargas Edith,Romero-Diaz Viktor

Abstract

Menkes disease (MD) is a rare and often lethal X-linked recessive syndrome, characterized by generalized alterations in copper transport and metabolism, linked to mutations in the ATPase copper transporting α (ATP7A) gene. Our objective was to identify genomic alterations and circulating proteomic profiles related to MD assessing their potential roles in the clinical features of the disease. We describe the case of a male patient of 8 months of age with silvery hair, tan skin color, hypotonia, alterations in neurodevelopment, presence of seizures, and low values of plasma ceruloplasmin. Trio-whole-exome sequencing (Trio-WES) analysis, plasma proteome screening, and blood cell migration assays were carried out. Trio-WES revealed a hemizygous change c.4190C > T (p.S1397F) in exon 22 of the ATP7A gene. Compared with his parents and with child controls, 11 plasma proteins were upregulated and 59 downregulated in the patient. According to their biological processes, 42 (71.2%) of downregulated proteins had a participation in cellular transport. The immune system process was represented by 35 (59.3%) downregulated proteins (p = 9.44 × 10−11). Additional studies are necessary to validate these findings as hallmarks of MD.

Funder

Consejo Nacional de Ciencia y Tecnología

Publisher

MDPI AG

Subject

Genetics(clinical),Genetics

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