# Novel coenzyme Q6 variant reveals non-immune determinants of survival during pneumococcal sepsis

> **NIH NIH R01** · WASHINGTON UNIVERSITY · 2024 · $739,362

## Abstract

1 PROJECT SUMMARY
 2 Sepsis caused by Streptococcus pneumoniae (Sp; the pneumococcus) causes significant morbidity and
 3 mortality, despite vaccines, antimicrobials, and supportive care. Sepsis is defined as “life-threatening organ
 4 damage due to a pathogen-driven, dysregulated immune response.” The immune-centric model posits that
 5 imbalances between pro- and anti-inflammatory immune mediators create a perfect septic storm of hyper-
 6 inflammation, tissue damage, and immuno-suppression. However, no immunomodulatory therapies have yet
 7 shown efficacy in improving mortality of sepsis. Our novel model of Sp sepsis prompts us to reconsider this
 8 immunocentric model. We found a novel single nucleotide variant (SNV) in the gene encoding co-enzyme Q6
 9 (COQ6) to be associated with susceptibility to Sp disease in an at-risk human population. The variant converts
10 an aspartate (D) to a tyrosine (Y) residue, and so we call the variant “DY” (COQ6-DY). We created the “DY
11 mouse” line, homozygous for the homologous Coq6-DY variant, which suffer increased mortality after Sp lung
12 infection. We then made chimeric mice to separate immune from non-immune cell dysfunction. Surprisingly,
13 recipient DY mice were more susceptible to Sp sepsis, despite reconstitution with wild-type (WT) immune cells.
14 Reconstitution of WT mice with DY immune cells improved survival after Sp infection. Our data reveal that non-
15 immune factors drive mortality during Sp sepsis, prompting re-evaluation of the immunocentric model of sepsis.
16 To explore why Coq6-DY increases Sp susceptibility, we tested how Coq6-DY disrupts COQ6 function.
17 Located in the inner mitochondrial membrane, COQ6 biosynthesizes the lipid ubiquinone (Q). Q serves as an
18 electron acceptor in the electron transport chain (ETC) during oxidative phosphorylation (OXPHOS). In health,
19 most tissues rely on OXPHOS for ATP generation. Infection induces metabolic remodeling and OXPHOS
20 downregulation, necessary to generate and sustain an anti-pathogen, pro-inflammatory response. Abnormal
21 metabolic remodeling may drive sepsis. In DY tissues, Q biosynthesis was intact, but OXPHOS downregulation
22 was accelerated in DY heart muscle after Sp challenge. Our proposal tests the hypothesis that aberrant
23 metabolic remodeling in DY mice causes hyperinflammation and increases organ damage in Sp sepsis through
24 three aims. First, we define the inflammatory and physiological derangements in Sp-infected DY recipients.
25 Second, we analyze metabolomic and single cell RNASeq profiles of infected DY recipients for predicted
26 correlations between metabolic abnormalities and pro-inflammatory transcriptional profiles. Finally, we test if
27 therapies chosen to counteract metabolic abnormalities in DY recipients improve survival in Sp sepsis. As an
28 Infectious Disease physician-scientist with expertise in cellular immunology, I am uniquely qualified to lead this
29 research. Our validated mouse mod...

## Key facts

- **NIH application ID:** 10945803
- **Project number:** 1R01HL177453-01
- **Recipient organization:** WASHINGTON UNIVERSITY
- **Principal Investigator:** Sharon Celeste Morley
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2024
- **Award amount:** $739,362
- **Award type:** 1
- **Project period:** 2024-08-26 → 2028-07-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10945803

## Citation

> US National Institutes of Health, RePORTER application 10945803, Novel coenzyme Q6 variant reveals non-immune determinants of survival during pneumococcal sepsis (1R01HL177453-01). Retrieved via AI Analytics 2026-05-25 from https://api.ai-analytics.org/grant/nih/10945803. Licensed CC0.

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