# CCN3-derrived peptides to treat liver injury

> **NIH NIH R41** · BLR BIO, LLC · 2020 · $56,824

## Abstract

Project Summary
Chronic liver disease is becoming a major public health issue with estimates of up to 40% prevalence of non-
alcoholic fatty liver disease (NAFLD) and 12% with non-alcoholic steatohepatitis (NASH) in the U.S. Liver disease
and cirrhosis was the 12th leading cause of mortality in the U.S. in 2014. Obesity and metabolic syndrome are
important causes of fatty liver disease or steatosis, with NAFLD rates of up to 70% in type 2 diabetic patients, and
30%-90% of those with obesity. It is also affecting children. NASH and liver fibrosis can lead to organ failure. The
estimated cost of NAFLD alone in the U.S., in direct medical costs are about $103 billion. There are currently no
drugs available to treat either steatosis or liver fibrosis.
In 2009 it was shown that the matricellular signaling protein CCN3 is a natural regulator, or balancer, of the well-
established pro-fibrotic protein and family member CCN2. The anti-fibrotic role of CCN3 and potential as a drug
was recently shown in treatment models of renal fibrosis driven by diabetes and obesity, and in models of skin
scarring. In the former, it showed the capacity to halt and even reverse established fibrosis. To create a more
effective drug, BLR Bio in a peptide discovery program, identified two critical regions on the CCN3 protein
responsible for this actively and has proposed stable synthetic peptides. Our long-term goal is to use these
improved drug forms to treat NAFLD, both reducing the mortality and morbidity associated the disease, and
dramatically curbing the growing healthcare costs.
Our preliminary experiments were carried out in a model of type 2 diabetes and obesity, a model we used to study
renal fibrosis. As part of those studies, we generated intriguing data suggesting that our lead peptide, BLR200
(BLR100 has not yet been tested), is able to block in a dose-dependent manner the upregulation of key selected
fibrosis genes in the liver, and the early manifestation of liver fibrosis. Surprisingly, it also blocked and perhaps
reversed steatosis in almost half of the animals.
In collaboration with liver experts at the University of Michigan, we aim to confirm proof of principle in animals.
Specifically, we will test and compare BLR100 and BLR200, for dose-response efficacy in the FATZO rodent model,
which on a high fat diet develops NAFLD and NASH-like pathology. We will define the two peptides’ ability to
block, and perhaps reverse, development of established liver injury (steatosis and its down-stream consequences
including inflammation, hepatocyte necrosis and fibrosis [NASH]). Controls will include mice on a normal chow
diet and placebo treated mice on the high fat diet. Parameter’s tested will be aligned to currently accepted clinical
measures of progression including biomarkers. Added will be a proteomic analysis to begin elucidating the
pathways involved. Completion of these milestones will set the stage for a Phase 2 STTR grant and partner
investment to complete ...

## Key facts

- **NIH application ID:** 10126319
- **Project number:** 3R41DK116448-01A1S1
- **Recipient organization:** BLR BIO, LLC
- **Principal Investigator:** BRUCE L RISER
- **Activity code:** R41 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $56,824
- **Award type:** 3
- **Project period:** 2020-04-01 → 2020-08-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10126319

## Citation

> US National Institutes of Health, RePORTER application 10126319, CCN3-derrived peptides to treat liver injury (3R41DK116448-01A1S1). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/10126319. Licensed CC0.

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