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Seung Kim, M.D., Ph.D.

Professor, Department of Developmental Biology and Medicine (Oncology Division)
Stanford University School of Medicine/HHMI
Investigator, HHMI

Beckman Center B300, 279 Campus Drive
Stanford, CA 94305-5329
USA

p. 650.723.6230
f. 650.725.7739
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Seung Kim, M.D., Ph.D. - Investigator Profile

Understanding organ development and achieving functional restoration of diseased organs is a broad goal motivating intensive effort in biomedical research. Many vital organs derive from the endodermal and mesodermal germ layers to form the gastrointestinal and respiratory tracts, yet little is known about the molecular and cellular programs that coordinate steps culminating in proper organ morphogenesis and axial position, cell differentiation, proliferation and physiologic function. Replacement or regeneration of pancreatic islets of Langerhans, endocrine organs that secrete insulin and glucagon, has emerged as a paradigm for organ restoration in recent years. Deficiency of insulin-producing islet beta-cells underlies the pathogenesis of diabetes mellitus, a disease with devastating autoimmune (type 1) and pandemic (type 2) forms. However, islet replacement in diabetes is ultimately limited by our inadequate understanding of mechanisms controlling islet formation and growth. Thus, islet replacement is a specific challenge to the consensus that knowledge about solid organ development and expansion can be used to restore organ function in human diseases.

To meet this challenge, my group has pioneered new approaches to create, expand, and regenerate islets. We discovered Drosophila endocrine cells, including insulin-producing cells, that are functional orthologs of mammalian islet cells, and generated novel genetic screens to identify evolutionarily conserved programs that control the development, expansion and reprogramming of islet cells. We identified new FACS-based methods to purify specific classes of cells that generate the pancreas and islets in mice and humans, including definitive endoderm and native pancreatic progenitor cells, providing a powerful platform to accelerate use of pancreatic and embryonic stem cells for islet studies and replacement. We elucidated new molecular pathways that control proliferation of beta-cells in physiological settings or islet tumors. We envision that modulation of these pathways will be useful for stimulating expansion of functional islets for diabetes, and for treating neuroendocrine cancer. Below, we summarize our major research efforts and describe how our unique approaches to islet and pancreas biology should culminate in diagnostic and therapeutic paradigms for human diseases.

Scientific Interests/Keywords

Pancreas developmental biology, diabetes, islet biology, genetics, epigenetics

Professor, Department of Developmental Biology and Medicine (Oncology Division), Kim Lab

Click to view the profile for Jonghyeob Lee, Ph.D..
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Publication Citation
22814600 Goodyer WR, Gu X, Liu Y, Bottino R, Crabtree GR, Kim SK Neonatal β Cell Development in Mice and Humans Is Regulated by Calcineurin/NFAT. (2012) Dev Cell 23: 21-34 (Added 2012-08-29 13:49:36.5118)
21993628 Chen H, Gu X, Liu Y, Wang J, Wirt SE, Bottino R, Schorle H, Sage J, Kim SK PDGF signalling controls age-dependent proliferation in pancreatic β-cells. (2011) Nature 478: 349-55 (Added 2013-03-25 17:11:01.821711)
21362573 Wang P, Rodriguez RT, Wang J, Ghodasara A, Kim SK Targeting SOX17 in human embryonic stem cells creates unique strategies for isolating and analyzing developing endoderm. (2011) Cell Stem Cell 8: 335-46 (Added 2011-08-02 10:37:15.085368)
20362535 McKnight KD, Wang P, Kim SK Deconstructing pancreas development to reconstruct human islets from pluripotent stem cells. (2010) Cell Stem Cell 6: 300-8 (Added 2011-02-23 20:05:53.078122)
19390090 Chen H, Gu X, Su IH, Bottino R, Contreras JL, Tarakhovsky A, Kim SK Polycomb protein Ezh2 regulates pancreatic beta-cell Ink4a/Arf expression and regeneration in diabetes mellitus. (2009) Genes Dev 23: 975-85 (Added 2010-07-31 23:43:11.620896)
17190805 Sugiyama T, Rodriguez RT, McLean GW, Kim SK Conserved markers of fetal pancreatic epithelium permit prospective isolation of islet progenitor cells by FACS. (2007) Proc Natl Acad Sci U S A 104: 175-80 (Added 2010-08-24 14:16:49.728952)
16988714 Heit JJ, Apelqvist AA, Gu X, Winslow MM, Neilson JR, Crabtree GR, Kim SK Calcineurin/NFAT signalling regulates pancreatic beta-cell growth and function. (2006) Nature 443: 345-9 (Added 2010-08-24 14:17:56.405344)
15372035 Kim SK, Rulifson EJ Conserved mechanisms of glucose sensing and regulation by Drosophila corpora cardiaca cells. (2004) Nature 431: 316-20 (Added 2010-08-24 14:16:01.969865)
Resource ID Name Contributed on Primary Contributor
4063 OE.Mouse.Neurog3.CMV Mar 28, 2011 Yes
4064 OE.Human.Neurogenin 3.CMV Mar 28, 2011 Yes
4066 OE.Human.NEUROG3.CMV Mar 28, 2011 Yes
4067 OE.Mouse.Pax4.CMV Mar 28, 2011 Yes
4069 OE.Mouse.Arx.CMV Mar 28, 2011 Yes
4070 OE.Mouse.Pdx1.CMV Mar 28, 2011 Yes
4071 OE.Human.NEUROG3.CMV Mar 28, 2011 Yes
4085 OE.Unclassified.eGFP.Human Insulin Apr 20, 2011 Yes
4118 Gene expression profiling of hESC derived eGFP-SOX17+ endoderm cells Aug 2, 2011 Yes
4257 Procedure for fractionating and isolating cell subsets from human fetal pancreas. Mar 1, 2012 Yes
4258 Procedure for assessing gene expression in cell subsets from the human fetal pancreas. Mar 1, 2012 Yes
4259 Procedures to assess gene expression changes in mouse fetal pancraetic cell subsets. Mar 1, 2012 Yes
4260 Procedure for fractionation and gene expression analysis of juvenile human islet cells. Mar 1, 2012 Yes
4261 Procedure for identifying chromatin in juvenile human islet cells. Mar 1, 2012 Yes
4287 Establish transgenic strains to lineage-trace beta- and alpha-cells in pregnant females Mar 15, 2012
4288 Procedures for Isolating and Characterizing the Function of Juvenile Human Islets Mar 15, 2012
4570 Procurement and shipment of human fetal pancreatic fragments Mar 5, 2013
17 completed resources viewable