# Carbonic Anhydrase 5A Dysfunction in Complex V Deficiency

> **NIH NIH R03** · CHILDREN'S HOSP OF PHILADELPHIA · 2020 · $132,000

## Abstract

ABSTRACT
Mitochondrial complex V (CV) subunit gene mutations cause a variety of severe metabolic diseases that impair
child health and development, with strokes, neuropathy, ataxia, vision loss, and cardiomyopathy. There is no
clinically-approved assay of CV function, therefore, making the diagnosis is challenging. The discovery that
metabolites downstream of Carbonic Anhydrase 5A (CA5A) are recurrently abnormal in patients with CV
deficiency has profound implications on developing targeted diagnostic testing for this profound energy
deficiency. We Hypothesize that (a) CV and Carbonic Anhydrase 5A (CA5A) physically associate, therefore,
mutations in CV cause CA5A deficiency and (b) scrutiny of the metabolites downstream of CA5A will provide
novel biomarkers for CV deficiency. Specific Aims of this work are to [Aim 1] Evaluate incidence of CV
deficiency among patients with a newborn screen consistent with CA5A deficiency; [Aim 2] Determine the
presence and degree of CA5A impairment in human fibroblast, cybrid and liver cell line models of CV disease;
and [Aim 3] Determine if there is a physical association between CA5A and CV. Methods will sequencing CV
subunit genes in subjects with abnormal newborn screens consistent with CA5A dysfunction (prospective and
retrospective cohort), direct measurement of CA5A function using stable isotope-labeled acetate and in vitro
cellular assessment of targeted and untargeted metabolites (Orbitrap liquid chromatography/mass
spectrometry) in fibroblasts and hepatic cell lines from healthy individuals, genetic-based CV diseases and
pharmacologic inhibition (oligomycin). Targeted metabolomics will focus on metabolites downstream of CA5A:
amino acids, particularly citrulline (ultra-high-performance liquid chromatrography) and the organic acids
propionic acid and hydroxyisovaleric acid (gas chromatography/mass spectrometry). determination of CA5A
function using stable isotope studies (13C-labeled acetate incubation, isotope-ratio mass spectrometry) in
transmitochondrial cybrid, hepatic and fibroblast cell lines from healthy individuals, genetic-based CV diseases
and pharmacologic CV inhibition (oligomycin). We will also investigate the in vitro physical interaction of CA5A
and CV (co-immunoprecipitation, blue native gel) in normal and genetic-based CV disease hepatocyte cell-
lines. These studies will rigorously investigate the interaction between CA5A function and CV
deficiency and new potential biomarkers for diagnosing CV disease. Our long-term goal is to expand the
diagnostic and treatment options available for human CV deficiency, for which no treatment currently exists.
These studies will establish the foundation of which to develop future clinical diagnostic assays to rapidly and
precisely diagnosis CV disease and will lead to a new understanding of the role of CV in coordinating
mitochondrial biochemical pathways, providing a novel target for future therapies.

## Key facts

- **NIH application ID:** 10042614
- **Project number:** 1R03DK125662-01
- **Recipient organization:** CHILDREN'S HOSP OF PHILADELPHIA
- **Principal Investigator:** Rebecca Ganetzky
- **Activity code:** R03 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $132,000
- **Award type:** 1
- **Project period:** 2020-07-15 → 2022-06-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10042614

## Citation

> US National Institutes of Health, RePORTER application 10042614, Carbonic Anhydrase 5A Dysfunction in Complex V Deficiency (1R03DK125662-01). Retrieved via AI Analytics 2026-05-26 from https://api.ai-analytics.org/grant/nih/10042614. Licensed CC0.

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