Savinov Lab

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Primary Research Focus

The Savinov Lab focuses on studying the underlying mechanisms controlling organ-specific autoimmune diseases such as type I diabetes (T1D). Progression of T1D involves the activation of autoimmune T cells, consequent homing of activated lymphocytes to the pancreatic islets, and ensuing destruction of insulin-producing beta cells.

Pathogenesis of type I diabetes (T1D) is driven by continuous destruction of insulin-producing β cells within the pancreatic islets, performed directly by autoreactive islet-specific T lymphocytes. The Savinov Lab current research projects are focused on the mechanisms involved in the regulation of T cell activation and tolerance in regard to T1D, even though most of them could take place in other autoimmune processes. Using genetic mouse models, and variety of primary and established cell lines, we are examining the molecular mechanisms leading to inefficient negative co-stimulation, a control mechanism for T cell activation by auto-antigens, along with some defects in the intracellular signaling cascades involved in the autoimmune process.

By determining how autoimmune T cells are initially activated during T1D pathogenesis, how they home to the target organ and how they destroy their beta cell targets, causing clinical onset of T1D, the Savinov Lab hopes to find an effective molecular therapy capable of controlling the autoimmune process.

Primary Research Group

Diabetes

Secondary Research Groups

(605) 312-6019

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About the Savinov Lab

About Alexei Savinov, Associate Scientist

Dr. Alexei Savinov is an experienced immunobiologist with a proven record in basic and translational studies focused on autoimmunity.

Dr. Savinov holds a Ph.D. in biochemistry from the Institute for Experimental Medicine in Leningrad. Before joining Sanford Research, Dr. Savinov held academic appointments at the Jackson Laboratory and at Sanford-Burnham Medical Research Institute.

Academic and Professional Affiliations

Academic Affiliations

  • Associate Professor of Pediatrics, University of South Dakota Sanford School of Medicine (2009-present)
  • Adjunct Assistant Professor of Biochemistry, South Dakota State University (2015-present)

Professional Affiliations

  • American Association for Immunologists
  • American Diabetes Association
  • Immunology of Diabetes Society

Highlighted Publications

Towards antigen-specific Tregs for type 1 diabetes: Construction and functional assessment of pancreatic endocrine marker, HPi2-based chimeric antigen receptor. Radichev IA, Yoon J, Scott DW, Griffin K, Savinov AY.  Cell Immunol. 2020 Dec;358:104224. doi: 10.1016/j.cellimm.2020.104224. Epub 2020 Sep 30. PubMed PMID: 33068914; PubMed Central PMCID: PMC7655659.

Self-Transducible Bimodal PDX1-FOXP3 Protein Lifts Insulin Secretion and Curbs Autoimmunity, Boosting Tregs in Type 1 Diabetic Mice. Amatya C, Radichev IA, Ellefson J, Williams M, Savinov AY. Molecular therapy: the journal of the American Society of Gene Therapy. 2018; 26(1):184-198. PubMed [journal] PMID: 28988715, PMCID: PMC5762970

The Type 1 Diabetes-Resistance Locus Idd22 Controls Trafficking of Autoreactive CTLs into the Pancreatic Islets of NOD Mice. Whitener RL, Gallo Knight L, Li J, Knapp S, Zhang S, Annamalai M, Pliner VM, Fu D, Radichev I, Amatya C, Savinov A, Yurdagul A Jr, Yuan S, Glawe J, Kevil CG, Chen J, Stimpson SE, Mathews CE. Journal of immunology (Baltimore, Md.: 1950). 2017; 199(12):3991-4000. NIHMSID: NIHMS913291 PubMed [journal] PMID: 29109122, PMCID: PMC5716886

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Awards

  • T. Denny Sanford Pediatric Collaborative Research Award, Sanford Health (2017)
  • Rachmiel Levine Scientific Achievement Award (2011)
  • Rachmiel Levine Scientific Achievement Award (2010)
  • Juvenile Diabetes Research Foundation Postdoctoral Fellowship Award (2001)
  • The Jackson Laboratory Postdoctoral Fellowship Award (1998)

Lab Projects and News

Is the heterogenic mother mitochondrial DNA genome a cause of reject in transplanted organs from cloned animals?

This is an investigation to understand if the use of organs from cloned animals in organ transplantation, specifically nuclear-mitochondrial incompatibilities, leads to organ rejection when organs from cloned animals are used for treating end-stage disease.

Genetic Regulation of Human Beta Cell Destruction

This research focuses on elucidating the mechanistic implications for the contribution of T1D-associated allelic variants during the activation and effector phases of CTL function.

Meet the Savinov Team

Prerana Sharma, MS

Research Specialist

Prerana Sharma joined the Savinov Lab in 2018 to assist the team in the investigation of the role of PTPN22 variants in type I diabetes-associated interaction between T cells and endothelial cells.

Prerana holds a master’s degree in biomedical engineering from the University of South Dakota.