Premature Ovarian Insufficiency in CLPB Deficiency: Transcriptomic, Proteomic and Phenotypic Insights

Overview

Journal J Clin Endocrinol Metab

Publisher Oxford University Press

Specialty Endocrinology

Date 2022 Sep 8

PMID 36074910

Authors

Elena J Tucker

Megan J Baker

Daniella H Hock

Julia T Warren

Sylvie Jaillard

Katrina M Bell

Rajini Sreenivasan

Shabnam Bakhshalizadeh

Chloe A Hanna

Nikeisha J Caruana

Saskia B Wortmann

Shamima Rahman

Robert D S Pitceathly

Jean Donadieu

Aurelia Alimi

Vincent Launay

Paul Coppo

Sophie Christin-Maitre

Gorjana Robevska

Jocelyn van den Bergen

Brianna L Kline

Katie L Ayers

Phoebe N Stewart

David A Stroud

Diana Stojanovski

Andrew H Sinclair

Affiliations

Soon will be listed here.

Abstract

Context: Premature ovarian insufficiency (POI) is a common form of female infertility that usually presents as an isolated condition but can be part of various genetic syndromes. Early diagnosis and treatment of POI can minimize comorbidity and improve health outcomes.

Objective: We aimed to determine the genetic cause of syndromic POI, intellectual disability, neutropenia, and cataracts.

Methods: We performed whole-exome sequencing (WES) followed by functional validation via RT-PCR, RNAseq, and quantitative proteomics, as well as clinical update of previously reported patients with variants in the caseinolytic peptidase B (CLPB) gene.

Results: We identified causative variants in CLPB, encoding a mitochondrial disaggregase. Variants in this gene are known to cause an autosomal recessive syndrome involving 3-methylglutaconic aciduria, neurological dysfunction, cataracts, and neutropenia that is often fatal in childhood; however, there is likely a reporting bias toward severe cases. Using RNAseq and quantitative proteomics we validated causation and gained insight into genotype:phenotype correlation. Clinical follow-up of patients with CLPB deficiency who survived to adulthood identified POI and infertility as a common postpubertal ailment.

Conclusion: A novel splicing variant is associated with CLPB deficiency in an individual who survived to adulthood. POI is a common feature of postpubertal female individuals with CLPB deficiency. Patients with CLPB deficiency should be referred to pediatric gynecologists/endocrinologists for prompt POI diagnosis and hormone replacement therapy to minimize associated comorbidities.

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