# Innate inflammation in osteoarthritis

> **NIH VA I01** · VA SAN DIEGO HEALTHCARE SYSTEM · 2020 · —

## Abstract

Osteoarthritis (OA) is a major cause of disability in the USA, particularly so in veterans, who are
disproportionately affected by aging and joint trauma. OA culminates in failure of the joint, which includes
compromised cartilage chondrocyte differentiation and function, by mechanisms that are not completely
understood. Because there is no disease-modifying medical therapy for OA, there is major unmet need to
advance translation. Our long-term objective is to validate novel targets to limit OA cartilage failure, including
processes that promote molecular innate inflammatory processes ("inflamm-aging"). A major obstacle in the
field is that multiple homeostasis mechanisms are dysfunctional in OA chondrocytes, and we need to sort out
which are the earliest, and central to the chondrocyte differentiation changes and viability loss. We have
identified decreased mitochondrial mass, function, and biogenesis capacity in aging and OA knee
chondrocytes, linked partly to deficiency of TFAM and other mitochondrial transcription factors. Our core
hypothesis is that articular chondrocyte mitochondrial dysfunction is an early, pivotal, targetable, and reversible
change in OA due to aging and biomechanical injury, and amplified by altered mitochondrial retrograde
signaling. This includes decrease in the anti-inflammatory mitochondrial peptide humanin, causing effects on
chondrocytes that we posit to be at least partly reversible in vitro using the humanin analog HNGF6A.
 Effective control of injury- and aging-associated tissue degeneration requires not only biogenesis but also
maintenance of healthy mitochondria. In the novel, testable OA pathogenesis model that we hypothesize,
chondrocyte mitochondrial damage is perpetuated, in large part, by feed-forward and feedback loops involving
compromise in cell surveillance mechanisms that normally assure mitochondrial quality control. We specifically
hypothesize the failure of chondrocyte mitophagy, via not only deficiency of the mitophagy “linchpin” BNIP3a,
but also decreased proteasomal degradation of damaged polyubiquitinated outer mitochondrial membrane
proteins, such as PINK1 and Parkin, by the ubiquitin proteasome system (UPS), which is essential for
mitophagy.
 Our preliminary studies break substantial new ground by revealing markedly impaired UPS function in
OA chondrocytes, including defective 20S proteasome core particle proteolytic activity, and accumulation of
chondrocyte K48 polyubiquitinated proteins. We further identified that human knee OA chondrocytes have
impaired assembly of the proteasome, a state that induces global outcomes of loss of chondrocytic
differentiation, via diminished expression of the chondrocyte master transcription factor Sox9, and decreased
matrix anabolic gene expression. For testing our integrative model of early, pivotal OA pathogenesis,
innovation is applied by our bringing together of a particularly diverse investigative team, including
collaborating experts in mitochondrial ...

## Key facts

- **NIH application ID:** 9898282
- **Project number:** 5I01BX001660-08
- **Recipient organization:** VA SAN DIEGO HEALTHCARE SYSTEM
- **Principal Investigator:** Robert A. Terkeltaub
- **Activity code:** I01 (R01, R21, SBIR, etc.)
- **Funding institute:** VA
- **Fiscal year:** 2020
- **Award amount:** —
- **Award type:** 5
- **Project period:** 2012-04-01 → 2021-09-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9898282

## Citation

> US National Institutes of Health, RePORTER application 9898282, Innate inflammation in osteoarthritis (5I01BX001660-08). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/9898282. Licensed CC0.

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