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1–2 minutes

Presenter Profile: Systemic Effects of Liver Senescence in Relation to Metabolic Disease

Kuo Du, PhD

Assistant Professor
University of Kansas Medical Center

Featured in the Session: Is Obesity Accelerated Aging? A Physiologic Perspective

When

Saturday, June 6
at 8:00 a.m.

Where

245 (Level 2)
Ernest N. Morial Convention Center

Kuo Du, PhD
Kuo Du, PhD

What is your presentation about?

My presentation explores how hepatocyte senescence drives metabolic liver disease and systemic dysfunction. I will show how senescent hepatocytes actively reshape both the liver and distant organs through senescence-associated secretory phenotype (SASP) signaling. By integrating molecular, animal, and human data, I highlight senescence as a key mechanism underlying metabolic dysfunction-associated steatotic liver disease (MASLD) progression. Finally, I discuss emerging strategies to target senescence as a novel therapeutic approach.

How do you hope your presentation will impact diabetes research or care?

I hope my presentation will highlight that over 65% of patients with type 2 diabetes have MASLD, a rapidly rising and clinically significant comorbidity. By linking hepatocyte senescence to systemic metabolic dysfunction, including pancreatic islet impairment, this work underscores the liver as a critical therapeutic target in diabetes. Ultimately, targeting liver senescence may offer new strategies to improve glycemic management and reduce diabetes-related complications.

How did you become involved with this area of diabetes research or care?

My research began with a focus on liver biology, but over time I became increasingly aware of how closely liver dysfunction is linked to type 2 diabetes in patients. Seeing that a large proportion of individuals with diabetes also have MASLD motivated me to better understand this connection. This led me to focus on hepatocyte senescence as a potential mechanism linking liver disease to systemic metabolic dysfunction.