Pipeline
We are pursuing drug development programs for a range of fibrotic diseases, focusing on tissue-specific integrin modulation and TGF-β1 signaling inhibition.
PLN-74809
Dual selective inhibitor of aVβ6/aVβ1
Idiopathic Pulmonary Fibrosis
Stage of Development
Primary Sclerosing Cholangitis
Stage of Development
COVID-19-Associated ARDS
Stage of Development
PLN-1474
Selective inhibitor of aVβ1
F3/F4 NASH – Associated Liver Fibrosis
Stage of Development
Program 3
Inhibitor of aVβ8
Oncology
Stage of Development
Program 4
Anti-integrin mAb
Muscular Dystrophies
Stage of Development
Early Stage
Undisclosed targets
Various
Stage of Development
Our lead program, PLN-74809, is a small-molecule, dual selective inhibitor of αVβ1 / αVβ6 for idiopathic pulmonary fibrosis (IPF) and primary sclerosing cholangitis (PSC). These integrins cause upstream activation of TGF-β1 in actively fibrotic tissue. Inhibition of these integrins will block TGF-β1 activation, thereby preventing the growth of fibrotic tissue within the lung and bile ducts. PLN-74809 is currently enrolling two Phase 2a trials in patients with IPF and one Phase 2a trial in patients with PSC.
Our second program, PLN-1474, is an oral, small-molecule, selective inhibitor of TGF-β activation by the integrin αVβ1 for the treatment of end-stage liver fibrosis in NASH. In October 2019, we entered into a license and collaboration agreement with Novartis for global rights to PLN-1474. We are currently conducting a phase 1 trial of PLN-1474 in healthy volunteers. After Phase 1, Novartis will assume responsibility for all future development, manufacturing and commercialization.
In addition to our clinical programs, we are developing two preclinical integrin-based programs. The first is our oncology program. In the tumor microenvironment, certain integrins, such as αVβ8, can be overexpressed, resulting in increased activation and signaling of TGF-β, leading to a strong anti-inflammatory effect and resistance to immuno-oncology therapies. We are targeting integrins such as αVβ8 with the goal of removing the anti-inflammatory effect and, ultimately, sensitizing tumors to checkpoint inhibitors.
Our second preclinical program, a monoclonal antibody being developed for treatment of muscular dystrophies, including Duchenne Muscular Dystrophy. We have identified an integrin receptor that appears to act as a natural compensatory mechanism in muscular dystrophy, helping preserve muscle function and slow deterioration. We have shown in animal models that by activating this receptor with an antibody, we are able to increase muscle strength and reduce muscle damage. Because the antibody is not mutation specific, it could potentially be effective as a single therapy or in combination with other treatments across multiple muscular dystrophy indications. This program is currently in the candidate selection phase of development.
Pliant Therapeutics, Inc.
260 Littlefield Avenue,
South San Francisco, CA 94080
info@pliantrx.com
650.481.6770