Racial inequities and rare CFTR variants: Impact on cystic fibrosis diagnosis and treatment

Malinda Wu; Jacob D. Davis; Conan Zhao; Tanicia Daley; Kathryn E. Oliver

Journal of Clinical & Translational Endocrinology (Jun 2024)

Racial inequities and rare CFTR variants: Impact on cystic fibrosis diagnosis and treatment

Malinda Wu,
Jacob D. Davis,
Conan Zhao,
Tanicia Daley,
Kathryn E. Oliver

Affiliations

Malinda Wu: Department of Pediatrics, Emory University School of Medicine, Atlanta, GA, USA; Pediatric Institute, Children’s Healthcare of Atlanta, Atlanta, GA, USA
Jacob D. Davis: Department of Biomedical Engineering, Georgia Institute of Technology and Emory University, Atlanta, GA, USA
Conan Zhao: Interdisciplinary Graduate Program in Quantitative Biosciences, Georgia Institute of Technology, Atlanta, GA, USA
Tanicia Daley: Department of Pediatrics, Emory University School of Medicine, Atlanta, GA, USA; Pediatric Institute, Children’s Healthcare of Atlanta, Atlanta, GA, USA
Kathryn E. Oliver: Department of Pediatrics, Emory University School of Medicine, Atlanta, GA, USA; Pediatric Institute, Children’s Healthcare of Atlanta, Atlanta, GA, USA; Corresponding author at: Emory University School of Medicine, Department of Pediatrics, 2015 Uppergate Drive NE, Atlanta, Georgia 30322, USA.

Journal volume & issue: Vol. 36
p. 100344

Abstract

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Cystic fibrosis (CF) has been traditionally viewed as a disease that affects White individuals. However, CF occurs among all races, ethnicities, and geographic ancestries. The disorder results from mutations in the CF transmembrane conductance regulator (CFTR). Varying incidence of CF is reported among Black, Indigenous, and People of Color (BIPOC), who typically exhibit worse clinical outcomes. These populations are more likely to carry rare CFTR variants omitted from newborn screening panels, leading to disparities in care such as delayed diagnosis and treatment. In this study, we present a case-in-point describing an individual of Gambian descent identified with CF. Patient genotype includes a premature termination codon (PTC) (c.2353C>T) and previously undescribed single nucleotide deletion (c.1970delG), arguing against effectiveness of currently available CFTR modulator-based interventions. Strategies for overcoming these two variants will likely include combinations of PTC suppressors, nonsense mediated decay inhibitors, and/or alternative approaches (e.g. gene therapy). Investigations such as the present study establish a foundation from which therapeutic treatments may be developed. Importantly, c.2353C>T and c.1970delG were not detected in the patient by traditional CFTR screening panels, which include an implicit racial and ethnic diagnostic bias as these tests are comprised of mutations largely observed in people of European ancestry. We suggest that next-generation sequencing of CFTR should be utilized to confirm or exclude a CF diagnosis, in order to equitably serve BIPOC individuals. Additional epidemiologic data, basic science investigations, and translational work are imperative for improving understanding of disease prevalence and progression, CFTR variant frequency, genotype-phenotype correlation, pharmacologic responsiveness, and personalized medicine approaches for patients with African ancestry and other historically understudied geographic lineages.

Published in Journal of Clinical & Translational Endocrinology

ISSN: 2214-6237 (Online)
Publisher: Elsevier
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the endocrine glands. Clinical endocrinology
Website: http://www.journals.elsevier.com/journal-of-clinical-and-translational-endocrinology/

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