• Microscopic view of blood with test tube.
  • The concept of health care in digital art

Mukherjee Lab

Advancing Diagnostic Competencies to Improve Patient Outcomes

About Our Lab

Our mission is to improve patient outcomes by investigating biomarkers associated with debilitating diseases and advancing their applications in diagnostics and therapeutics. By focusing on these biomarkers, we aim to predict, identify, understand, and guide the treatment of diseases. To achieve these goals, we analyze human biological fluids and tissue samples. We apply both established and novel bioanalytical technologies to identify and validate key biomarkers. Additionally, we employ in vitro, ex vivo, and in vivo experimental models to uncover molecular mechanisms and discover potential therapeutic targets.

Current projects

blood sample and urine collection tubes and supplies with requisition form for analysis in the clinical laboratory. Blood tubes and urine of patient with test report for analysis in the Hematology lab

Translational Biomarker Discovery and Validation

We are developing robust bioanalytical methodologies and statistically validated, combinatorial platforms that can identify and validate biomarkers as potential diagnostic candidates and/or therapeutic targets. Our ongoing investigations focus on renal diseases, diabetes, and cardiometabolic kidney syndrome.
Diagnostics and testing in the clinic

Developing CLIA-Compliant Laboratory-Developed Tests

Aligned with our mission to advance scientific discoveries from the bench to the clinic, the SIDD Clinical Laboratory—an integral part of the Mukherjee Lab—is leading efforts to transition biomarker-based tests into CLIA-compliant laboratory-developed tests (LDTs). This UTMB-wide initiative is a SIDD-led collaboration involving scientists, clinicians, and laboratory services. Our current pipeline includes tests targeting kidney diseases and cardiometabolic kidney syndrome.

Publications

The D2D3 form of uPAR acts as an immunotoxin and may cause diabetes and kidney disease

Soluble urokinase plasminogen activator receptor (suPAR) is a risk factor for kidney diseases. In addition to suPAR, proteolysis of membrane-bound uPAR results in circulating D1 and D2D3 proteins. We showed that when exposed to a high-fat diet, transgenic mice expressing D2D3 protein developed progressive kidney disease marked by microalbuminuria, elevated serum creatinine, and glomerular hypertrophy. D2D3 transgenic mice also exhibited insulin-dependent diabetes mellitus evidenced by decreased...

The D2D3 form of uPAR acts as an immunotoxin and may cause diabetes and kidney disease

Soluble urokinase plasminogen activator receptor (suPAR) is a risk factor for kidney diseases. In addition to suPAR, proteolysis of membrane-bound uPAR results in circulating D1 and D2D3 proteins. We showed that when exposed to a high-fat diet, transgenic mice expressing D2D3 protein developed progressive kidney disease marked by microalbuminuria, elevated serum creatinine, and glomerular hypertrophy. D2D3 transgenic mice also exhibited insulin-dependent diabetes mellitus evidenced by decreased...

The D2D3 form of uPAR acts as an immunotoxin and may cause diabetes and kidney disease

Soluble urokinase plasminogen activator receptor (suPAR) is a risk factor for kidney diseases. In addition to suPAR, proteolysis of membrane-bound uPAR results in circulating D1 and D2D3 proteins. We showed that when exposed to a high-fat diet, transgenic mice expressing D2D3 protein developed progressive kidney disease marked by microalbuminuria, elevated serum creatinine, and glomerular hypertrophy. D2D3 transgenic mice also exhibited insulin-dependent diabetes mellitus evidenced by decreased...

The D2D3 form of uPAR acts as an immunotoxin and may cause diabetes and kidney disease

Soluble urokinase plasminogen activator receptor (suPAR) is a risk factor for kidney diseases. In addition to suPAR, proteolysis of membrane-bound uPAR results in circulating D1 and D2D3 proteins. We showed that when exposed to a high-fat diet, transgenic mice expressing D2D3 protein developed progressive kidney disease marked by microalbuminuria, elevated serum creatinine, and glomerular hypertrophy. D2D3 transgenic mice also exhibited insulin-dependent diabetes mellitus evidenced by decreased...

The D2D3 form of uPAR acts as an immunotoxin and may cause diabetes and kidney disease

Soluble urokinase plasminogen activator receptor (suPAR) is a risk factor for kidney diseases. In addition to suPAR, proteolysis of membrane-bound uPAR results in circulating D1 and D2D3 proteins. We showed that when exposed to a high-fat diet, transgenic mice expressing D2D3 protein developed progressive kidney disease marked by microalbuminuria, elevated serum creatinine, and glomerular hypertrophy. D2D3 transgenic mice also exhibited insulin-dependent diabetes mellitus evidenced by decreased...

The D2D3 form of uPAR acts as an immunotoxin and may cause diabetes and kidney disease

Soluble urokinase plasminogen activator receptor (suPAR) is a risk factor for kidney diseases. In addition to suPAR, proteolysis of membrane-bound uPAR results in circulating D1 and D2D3 proteins. We showed that when exposed to a high-fat diet, transgenic mice expressing D2D3 protein developed progressive kidney disease marked by microalbuminuria, elevated serum creatinine, and glomerular hypertrophy. D2D3 transgenic mice also exhibited insulin-dependent diabetes mellitus evidenced by decreased...

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