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INFORMATION FOR

    Vijayakumar Kakade, PhD

    Research Scientist, Internal Medicine (Nephrology)
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    Research Scientist, Internal Medicine (Nephrology)

    Biography

    Dr. Kakade received his Ph.D in Biochemistry from University of Mysore, India. After completing his Ph.D, he entered a postdoctoral training at University of Kansas Medical Center, Kansas City, where his research focused on defining the candidate signals and sensors that regulate cell activation states in polycystic kidney disease. Dr. Kakade joined Yale University in 2016 where he established his research on the delineating the role of macrophages in cystogenesis in polycystic kidney disease and application of Imaging Mass Cytometry to understand the cell-cell interactions and cellular response involved in pathogenesis of human kidney diseases.

    Appointments

    Other Departments & Organizations

    Education & Training

    PhD
    University of Mysore, Biochemistry (2013)

    Research

    Overview

    The research goal is to understand the pathogenesis of polycystic kidney disease (PKD), a genetic disorder caused by mutations in either Pkd1 or Pkd2 genes, which encode polycystin 1 (PC1) and polycystin 2 (PC2) respectively, affecting the normal architecture of renal tubule, giving rise to ADPKD. Studies have uncovered the critical roles of polycystins and cilia in maintaining the three-dimensional structure of renal tubules. Understanding the mechanism and discovery of molecular determinants of cyst development and disease progression will advance the mechanism-based therapeutic target for the treatment of ADPKD. We have focused these efforts on delineating the role of Mcp1 in promoting macrophage-dependent cyst expansion in PKD and found that proinflammatory macrophages accumulate around the cyst and promote tubular epithelial cell injury. Subsequent switch to an alternative activation of macrophages promotes accelerated cyst growth due to an increase in tubular proliferative rates. High-resolution multiphoton imaging at the earliest phases of cyst formation following knock-out of Pkd1 showed that tubule dilation and epithelial proliferation occur simultaneously, and that dilation was more evident in tubules in which epithelial area had not increased implying proliferation is not a solitary force for tubule expansion. We are investigating the mechanism and the critical events that maintain the normal architecture of renal tubules and identify the critical components that are dysregulated in the absence of polycystins.

    Imaging mass cytometry (IMC) is a technique that uses a high-resolution laser combined with a mass cytometer to detect the presence, location, and amount of up to 42 different heavy metal conjugated antibodies hybridized onto a tissue section. Our group has successfully developed IMC and a machine learning algorithm to identify resident kidney cell populations, infiltrating cell populations, and cell activation and injury states in human kidney tissue. Research is focused on the application of IMC and the analysis pipeline for 2D quantitative assessment of cell location, cell-cell interactions, and cellular responses in human kidney diseases.

    Medical Research Interests

    Epithelial Cells; Kidney; Kidney Tubules; Macrophages; Nephrology; Polycystic Kidney, Autosomal Dominant; Spatial Analysis

    Research at a Glance

    Yale Co-Authors

    Frequent collaborators of Vijayakumar Kakade's published research.

    Publications

    2024

    2016

    Academic Achievements & Community Involvement

    • activity

      Frontiers in Medicine

    • activity

      Journal of Biomedical Nanotechnology

    • activity

      Journal of Kidney

    • honor

      CSIR-Senior Research Fellow

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