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Stefan Somlo, MD

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C. N. H. Long Professor of Medicine (Nephrology) and Professor of Genetics

Titles

Chief, Section of Nephrology

About

Titles

C. N. H. Long Professor of Medicine (Nephrology) and Professor of Genetics

Chief, Section of Nephrology

Appointments

Education & Training

Fellow
Yale University School of Medicine (1991)
Intern/Resident
Albert Einstein College of Medicine (1987)
MD
College of Physicians and Surgeons, Columbia University (1984)
AB
Harvard College, Biochemistry (1980)

Research

Overview

The primary focus of our laboratory is understand the pathogenesis of polycystic kidney and liver diseases (ADPKD, PCLD, ARPKD). These diseases are the most prominent among a larger group of pleiotropic human genetic diseases which share fibrocystic deterioration of the kidney and liver as a key phenotypic feature and whose pathogenesis is related to the functioning of the primary cilium and basal body complex. Study of these diseases have uncovered the central role of cilia in novel signaling pathways and in establishing and maintaining three dimensional tissue structure. Therefore, understanding the mechanism of polycystic diseases will not only shed light on diseases for which there are no therapies currently but will also uncover general principles of the functioning of cilia in human biology.

We have taken a longitudinal approach to understanding the pathogenesis of polycystic kidney disease beginning with discovery of human disease genes for ADPKD (PKD2), ARPKD (PKHD1) and six genes for isolated dominant polycystic liver disease. While we continue our gene discovery efforts using next generation sequencing approaches (whole exome sequencing), our lab now seeks to define the cellular pathways in which the ADPKD-gene products (PKD1, PKD2) function and to translate these findings to treatments for ADPKD. A central principle of our current approach is need to address disease molecular processes impacting polycystic kidney and liver diseases using novel genetically engineered mouse models. To this end, we have developed a series of conditional and inducible mouse models of the relevant human disease genes and combined them with bacterial artificial chromosome (BAC) transgenic lines modified by recombineering to define the mechanisms of ADPKD, PCLD and ARPKD in vivo. Specific projects include dissection of the molecular pathways of trafficking of PKD1 and PKD2, to cilia, the inter-relationship of cilia function with PKD1 and PKD2 signaling, and the interaction of polycystic diseases with the unfolded protein response. We continue to keep in focus the need to develop principles to guide therapy in ADPKD based on basic science discoveries.

Medical Subject Headings (MeSH)

Cilia; Genetics; Kidney Diseases; Liver Diseases; Nephrology; TRPP Cation Channels

Research at a Glance

Yale Co-Authors

Frequent collaborators of Stefan Somlo's published research.

Publications

2024

2023

2022

Clinical Trials

Current Trials

Clinical Care

Overview

Stefan Somlo, MD, specializes in nephrology and genetics. In his clinical practice, he treats acute and chronic kidney conditions, including end-stage renal disease and acute kidney injury, and electrolyte disorders such as hypernatremia, hypokalemia, and hyponatremia in the hospital setting. He is the chief of the Section of Nephrology.

Dr. Somlo's research focuses on the study of autosomal dominant polycystic kidney disease (ADPKD) and polycystic liver diseases. He has received funding from the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) and the Congressionally Directed Medical Research Programs (CDMRP).

Dr. Somlo is the C. N. H. Long Professor of Medicine (Nephrology) and a Professor of Genetics at Yale University School of Medicine.

Clinical Specialties

Internal Medicine; Nephrology

Fact Sheets

Board Certifications

  • Internal Medicine

    Certification Organization
    AB of Internal Medicine
    Original Certification Date
    1988

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