About Me
As a rheumatologist at ºÙºÙÊÓƵ, I am dedicated to understanding and addressing the unique needs, desires, and concerns of my patients. My fascination with science and the human narrative fuels my commitment to use my knowledge to restore health and wellbeing. My primary focus is on treating patients with rheumatoid and psoriatic arthritis, lupus, autoimmune vasculitis, osteoarthritis, osteoporosis, and particularly gout and other crystal-driven diseases.
I bring a wealth of experience and credentials to my role at ºÙºÙÊÓƵ. My specialty lies in managing complex autoimmune diseases and joint problems. I employ a variety of treatments, including immune system-modulating medications and joint and soft tissue injections. My dedication to proactive healthcare engagement and patient wellness is evident in my treatment approach, which is informed by scientific knowledge and a deep understanding of my patients’ unique circumstances.
Throughout my career, I have been privileged to witness the transformative power of advanced treatments in rheumatology. One of my most impactful experiences involved a patient with severe rheumatoid arthritis who was able to resume her career as a hairdresser after we introduced a new biologic therapy. These moments underscore the importance of staying abreast of medical advancements, a commitment I uphold in my practice.
My journey into medicine was inspired by my passion for science and stories. I studied biochemistry and English and American literature in college, finding in medicine a discipline where I could apply my scientific knowledge and my passion for understanding the human experience. I was drawn to rheumatology by the quality of my mentors, the challenges of my patients’ illnesses, and the intriguing ways in which the body’s immune defenses can sometimes cause harm to itself. As the founding director of the ºÙºÙÊÓƵ Crystal Diseases Study Group and co-director of the ºÙºÙÊÓƵ Gout Treatment Center, I am able to contribute to the field of rheumatology through both clinical care and research.
Conditions and Treatments
Credentials
Positions
- Professor,
- Professor,
- Director, Clinical and Translational Science Institute Education and Careers Unit
- Chief of Rheumatology, VA NY Harbor Health Care System
- Director, Rheumatology Fellowship Program
Board Certifications
- American Board of Internal Medicine (Rheumatology), 1992
Education and Training
- Fellowship, NYU School of Medicine, Rheumatology, 1993
- Residency, Jacobi Medical Center/Albert Einstein College of Medicine, Internal Medicine, 1990
- MD from New York University, 1987
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Insurance Plans Accepted
Please call the office for information about accepted insurance plans.
Michael H. Pillinger, MD does not accept insurance.
Research My Research
Interests
signal transduction and the regulation of cells involved in inflammation and rheumatoid arthritis
Research Summary
In rheumatoid arthritis (RA) the tissues of the involved joints assume inflammatory, autoimmune and pseudoneoplastic features. The cells contributing to these phenotypes include neutrophils, which accumulate in the RA joint space, and synovial fibroblasts (SFs), which proliferate in great numbers in the RA synovium (pannus) and secrete matrix metalloproteinases (MMPs) that participate in the destruction of cartilage.
The mitogen-activated protein kinases (MAPKs) include the Erks, Jnks and p38. Our laboratory is interested in the role of MAPKs on neutrophils and SF regulation. We are especially interested in the role of Erks. We have observed that, in neutrophils, Erk is rapidly activated in response to chemoattractants and regulates neutrophil adhesion, a critical early step in the acute inflammation. In SFs we have shown that Erk regulates proliferation, but also the release of some (MMP-1,3,9) but not other (MMP-13) metalloproteinases. Interestingly, high-dose salicylates (doses achievable in patients but in excess of those needed to inhibit cyclooxygenase) inhibit Erk in both neutrophils and SFs, and concordantly inhibit neutrophil adhesion and SF MMP release. Non-salicylate nonsteroidals also inhibit cyclooxygenase but do not reproduce these effects. Indeed, COX inhibition actually leads to enhancement of MMP release from synovial fibroblasts.
Our present aims are threefold: 1) to understand the mechanisms through which Erk positively regulates neutrophil adhesion; 2) to understand the cross talk between prostaglandin production and Erk activation in SF responses; 3) to understand the mechanisms through which salicylates inhibit Erk, as a clue into how Erk, and other signaling pathways, may be pharmacologically targeted. A better understanding of these phenomena may lead to new approaches, and new agents, for the treatment of RA.}
Research Interests Timeline
Clinical Trials and Research Studies
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A Multi-Center Phase 2/3 Randomized Double-Blind Placebo-Controlled Parallel- Group Safety and Efficacy Study of Dapansutrile Tablets in Subjects with an Acute Gout Flare
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Rheumatology SAMPLE (Specimen And Matched Phenotype Linked Evaluation) Registry and Biorepository
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Endothelial Activation in Gout: Early Markers for Cardiovascular Risk
Publications
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Helget, Lindsay N; Davis-Karim, Anne; O'Dell, James R; Mikuls, Ted R; Newcomb, Jeff A; Androsenko, Maria; Brophy, Mary T; England, Bryant R; Ferguson, Ryan; Pillinger, Michael H; Neogi, Tuhina; Wu, Hongsheng; Palevsky, Paul M
American journal of kidney diseases. 2024 Nov ; 84(5):538-545
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Barry, Austin; Helget, Lindsay N; Androsenko, Maria; Wu, Hongsheng; Kramer, Bridget; Newcomb, Jeff A; Brophy, Mary T; Davis-Karim, Anne; England, Bryant R; Ferguson, Ryan; Pillinger, Michael H; Neogi, Tuhina; Palevsky, Paul M; Merriman, Tony R; O'Dell, James R; Mikuls, Ted R
Arthritis & rheumatology. 2024 Oct ; 76(10):1552-1559
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Talmor, Nina; Pillinger, Michael H; Xia, Yuhe; Leonard, Ana; Curovic, Fatmira; Shah, Binita
Journal of the American Heart Association. 2024 Oct ; 13(19):e036701