John Turk, M.D., Ph.D.

John Turk, M.D., Ph.D.

Professor of Medicine
Director, Mass Spectrometry Resource

Office Location:		Southwest Tower, Room 855
Mailing Address:		Washington University School of Medicine 660 S. Euclid Ave. WUMS Box 8127 St. Louis, MO 63110
Telephone:		(314) 362-8190
Fax:		(314) 362-7641
E-mail Address:

Biography

EDUCATION
A.B., Washington University, 1970
M.D., Ph.D., Washington University School of Medicine, 1976
Intern in Internal Medicine, University of Chicago, 1976-1977
Resident in Laboratory Medicine, Washington University, 1977-1978
Resident in Internal Medicine, Washington University, 1978-1980
Fellow in Clinical Pharmacology, Vanderbilt University, 1980-1982

ACADEMIC POSITIONS/EMPLOYMENT

1982-1986	Assistant Professor of Medicine, of Pharmacology, and of Pathology, Washington University, St. Louis, MO
1986-1987	Associate Director of Exploratory Clinical Pharmacology, Ciba-Geigy Corporation, Pharmaceuticals Division, Summit, NJ
1988-1994	Associate Professor of Medicine and of Pathology, Washington University, St. Louis, MO
1994-present	Professor of Medicine and of Pathology, Washington University, St. Louis, MO

Research Interests

The hypothesis that a pancreatic islet Ca²⁺-independent phospholipase A₂ (iPLA₂β) is activated by secretagogues and that its products participate in b-cell signaling is being pursued with recently developed tools, including insulinoma cells with stably altered iPLA₂β expression that exhibit secretory and proliferative properties and sensitivities to Endoplasmic Reticulum (ER) stress that correlate with iPLA₂βb expression level. New ESI/MS/MS methods for lipid analyses reveal that iPLA₂β overexpression enhances stress-induced ceramide accumulation and increases lysophosphatidylcholine (LPC) levels. New proteomics tools reveal that β-cells proteolytically remove an iPLA₂β inhibitory domain and that iPLA₂β hydrolyzes its inhibitor BEL to an intermediate that alkylates cysteine. New iPLA₂β fluorescent constructs reveal that iPLA₂β translocates to perinuclear membranes in stimulated β-cells, and it interacts with Ca²⁺/calmodulin-dependent protein kinase IIb. Recently generated iPLA₂β-null mice have reduced male fertility and impaired macrophage NO synthase induction and become more glucose intolerant than wild-type mice on a high-fat diet. The emphasis is now shifting to in vivo studies, but work continues on Aims to: 1.) Characterize insulinoma cells with altered iPLA₂β or g expression with respect to secretion, proliferation, ER stress, and ion channel function; 2.) Characterize diet-induced changes in b-cell and tissue desaturases and lipids; 3.) Characterize iPLA₂β protein modifications; 4.) Conduct cell biologic studies of iPLA₂β isoform-specific organelle association and protein interactions; and 5.) Characterize genetically modified mice with altered iPLA₂ expression. With iPLA₂β-null and transgenic mice, insulin sensitivity and secretion are being examined in vivo, as are dietary effects on glucose-tolerance, body composition, and mortality; macrophage sensitivity to cholesterol-induced apoptosis; and atherogenesis in apoE^-/-/iPLA₂β^-/- double knockout mice. Goals also include preparing mice with tissue-specific alterations of iPLA₂β expression or altered iPLA₂γ expression. The public health relevance is that manipulating iPLA₂ expression might be useful in genetic engineering of β-cell lines for Type I diabetes mellitus (DM) cellular replacement therapy, and mechanisms to expand β-cell mass and improve insulin secretion in Type II DM could also be identified. Studies with iPLA₂β-null mice could also provide evidence that iPLA₂β pharmacologic inhibitors might have beneficial therapeutic effects, and our iPLA₂β inactivation studies might provide insight into inhibitor design.

Awards and Honors

1.	National Merit Scholarship, 1966-1970
2.	National Merit Scholarship, 1966-1970
3.	Wallace Award in History, Washington University, 1968
4.	Elected to Phi Beta Kappa honor society, Washington University, 1969
5.	National Science Foundation Undergraduate Research Fellowship, 1969
6.	A.B. summa cum laude, Washington University, 1970
7.	Medical Scientist Training Program Award, Washington University, 1970-1976
8.	Cori Award in Biological Chemistry, Washington University School of Medicine, 1972
9.	Elected to Alpha Omega Alpha honor society, Washington University, 1975
10.	Career Development Award, Pharmaceutical Manufacturer's Association, 1983-1985
11.	Research Career Development Award, National Institutes of Health, 1987-1992
12.	Elected to American Society for Clinical Investigation honor society, 1991
13.	Study Section Membership, National Institutes of Health, 1992-1996
14.	MERIT Award, National Institutes of Health, 1993-2001
15.	Elected to Association of American Physicians honor society, 2001
16.	MERIT Award, National Institutes of Health, 2001-2011
17.	Appointed to the Editorial Board, Journal of Biological Chemistry, 2007-2012