James A. Shayman

Add links
From Wikipedia, the free encyclopedia
James A. Shayman
Born
James Alan Shayman
Occupation(s)Physician scientist, nephrologist, and pharmacologist
Academic background
Alma materCornell University
Washington University School of Medicine
Academic work
InstitutionsUniversity of Michigan Medical School
Veterans Administration Medical Center

James Alan Shayman is an American physician scientist, nephrologist, and pharmacologist. He is Professor of Internal Medicine and Pharmacology and the Agnes C. And Frank D. McKay Professor at the Medical School of the University of Michigan.[1] He also serves as a staff nephrologist at the Ann Arbor Veterans Administration Medical Center.[2]

Shayman's research interests span the study of lysosomal biology and related disorders. His group is most known for the development of small-molecule inhibitors of glycosphingolipid synthesis and their use in lysosomal glycosphingolipid storage disorders. His team also discovered and characterized a novel lysosomal phospholipase A2, PLA2G15 and is investigating its role in phospholipidosis. He has published over 160 articles.[3]

Shayman is a Fellow of the American Heart Association and American Society of Nephrology as well as a Life Fellow of Clare Hall at the University of Cambridge. He has served as an Associate Editor for the Journal of Clinical Investigation and Translational Research and is serving in the same role for the Journal of the American Society of Nephrology.[4]

Education and early career[edit]

Shayman obtained a Bachelor of Arts degree from Cornell University in 1976, and received an M.D. in 1980 from Washington University in St. Louis. From July 1980 to June 1983, he served as a house officer in Medicine at Barnes Hospital in St. Louis, Missouri. Beginning in 1983, he pursued a Postdoctoral Fellowship with a specialization in Nephrology and Pharmacology under the mentorship of Aubrey Morrison and Oliver H. Lowry at Washington University School of Medicine in St. Louis.[5]

Career[edit]

Following his post-doctoral fellowship training, in 1985, Shayman began his academic career as an instructor in the Renal department of Washington University School of Medicine. He was recruited to the University of Michigan where from 1986 to 1992 he was appointed as assistant professor in the Department of Internal Medicine, Division of Nephrology. He subsequently was promoted to the positions of associate professor in 1992 and professor in 1997, respectively with a secondary appointment in Pharmacology. He has been serving as the Agnes C. and Frank D. McKay Professor.[1]

Shayman was the Associate Chair for Research Programs at the Department of Internal Medicine and Associate Vice President for Research in Health Sciences of the University of Michigan.[6] In addition, he has been serving as a staff nephrologist Veterans Administration Medical Center in Michigan.[2]

Research[edit]

Shayman's research is focused on lysosomal biology, the pathophysiology of traditional lysosomal storage disorders, and the role of the lysosome in more prevalent diseases including diabetes mellitus and polycystic kidney disease. A particular emphasis has been on the development of drug therapeutics for disorders of glycosphingolipid metabolism. This work has resulted in several patents including "Amino ceramide-like compounds and therapeutic methods of use"[7] and "Pyridine inhibitors of glucosylceramide synthase and therapeutic methods using the same."[8]

Substrate reduction therapy[edit]

An early collaboration with Norman Radin focused on substrate reduction as an alternative to enzyme replacement therapy for the treatment of lysosomal disorders such as Gaucher disease. It was suggested that substrate reduction posits that inhibition of metabolites that accumulate in the lysosome due to the loss of activity of a specific hydrolase can be treated with reversible inhibitors of specific anabolic enzymes. Following an early collaboration with Radin, the Shayman group went on to develop inhibitors of glucosylceramide synthase followed by proof of concept studies in models of Gaucher and Fabry disease that experimentally established the viability substrate reduction therapy.[9][10] Although this concept was initially met with skepticism from the academic and pharmaceutical communities, these compounds were eventually licensed to the Genzyme Corporation for clinical development in 2000. In 2014 eliglustat tartrate was approved by the Food and Drug Administration and the European Medicines Association. Eliglustat tartrate was the first orally bioavailable agent approved as the first stand-alone substrate reduction therapy for Gaucher disease type 1.[11][12]

Glycosphingolipid synthesis inhibitor[edit]

Shayman's work on developing the "first in class" glycosphingolipid synthesis inhibitor led to the consideration of whether more common disorders might be amenable to targeting glucosylceramide synthase.[13] Based on fundamental studies by his group and others demonstrating a role for glucosylceramide metabolism in conditions associated with aerobic glycolysis,[14] including diabetes[15] and polycystic kidney disease, glucosylceramide synthase inhibitors have been the focus of preclinical and clinical studies evaluating the potential for extended use applications of eliglustat and related compounds.[16]

Brain penetrant glycolipid synthesis inhibitors[edit]

In collaboration with Scott D. Larsen, Shayman's work has also been directed toward the identification of brain-penetrant glycolipid synthesis inhibitors for the treatment of Gaucher disease types 2 and 3,[17] GM2 gangliosidoses including Tay-Sachs and Sandhoff disease, and GM1 gangliosidosis.[18] Using computational analysis comparing eliglustat to known CNS penetrant compounds, novel glucosylceramide synthase inhibitors were designed around the eliglustat pharmacophore, demonstrating the lower glucosylceramide and ganglioside levels within the brain.[19]

Vasculopathy of fabry disease[edit]

The Shayman group has worked on the elucidation of the mechanisms underlying the vasculopathy of Fabry disease. His initial work led to the identification of three inducible models of vascular disease in the alpha-galactosidase A knockout mouse.[20] These models included oxidant-induced arterial thrombosis, accelerated atherogenesis, and impaired arterial relaxation. Both decreased nitric oxide bioavailability[21] and endothelial nitric oxide synthase uncoupling have been demonstrated to underlie these abnormalities. The insights led to identifying 3-nitrotyrosine as a biomarker for endothelial dysfunction in both experimental models and patients affected by classic forms of Fabry disease.[22][23]

PLA2GXV[edit]

Attempts to delineate potential off-target effects of eliglustat led to the discovery of a novel lysosomal hydrolase, phospholipase A2 group XV (PLA2GXV). This enzyme was initially identified as a transacylase and named 1-O-acylceramide synthase.[24] PLA2GXV is 50 percent identical to LCAT. In collaboration with John Tesmer and colleagues, the structure of PLA2GXV and, by extension, of lecithin cholesterol acyltransferase (LCAT) were solved. Mice engineered to be deficient in PLA2GXV developed a pulmonary phenotype associated with the conversion of alveolar macrophages to foam cells, a phenotype that resembles amiodarone toxicity.[25] A 2021 work has also identified PLA2GXV as the site of action for many drugs that cause a form of toxicity termed phospholipidosis.[26]

Awards and honors[edit]

Bibliography[edit]

Selected books[edit]

  • Renal Pathophysiology (1995) ISBN 978-0397513727
  • Essentials of Internal Medicine (2000) ISBN 978-0781719377

Selected articles[edit]

  • Rani CS, Abe A, Chang Y, Rosenzweig N, Saltiel AR, Radin NS, and Shayman JA. Cell cycle arrest induced by an inhibitor of glucosylceramide synthase. Correlation with cyclin-dependent kinases. J Biol Chem. 1995;270(6):2859-67.
  • Abe A, Shayman JA, and Radin NS. A novel enzyme that catalyzes the esterification of N-acetylsphingosine. Metabolism of C2-ceramides. J Biol Chem. 1996;271(24):14383-9.
  • Abe A, and Shayman JA. Purification and characterization of 1-O-acylceramide synthase, a novel phospholipase A2 with transacylase activity. J Biol Chem. 1998;273(14):8467-74.
  • Lee L, Abe A, and Shayman JA. Improved inhibitors of glucosylceramide synthase. J Biol Chem. 1999;274(21):14662-9.
  • Abe A, Gregory S, Lee L, Killen PD, Brady RO, Kulkarni A, and Shayman JA. Reduction of globotriaosylceramide in Fabry disease mice by substrate deprivation. J Clin Invest. 2000;105(11):1563-71.
  • Hiraoka M, Abe A, and Shayman JA. Cloning and characterization of a lysosomal phospholipase A2, 1-O-acylceramide synthase. J Biol Chem. 2002;277(12):10090-9.
  • Eitzman DT, Bodary PF, Shen Y, Khairallah CG, Wild SR, Abe A, Shaffer-Hartman J, and Shayman JA. Fabry disease in mice is associated with age-dependent susceptibility to vascular thrombosis. J Am Soc Nephrol. 2003;14(2):298-302.
  • Hiraoka M, Abe A, and Shayman JA. Structure and function of lysosomal phospholipase A2: identification of the catalytic triad and the role of cysteine residues. J Lipid Res. 2005;46(11):2441-7.
  • Abe A, Hiraoka M, and Shayman JA. A role for lysosomal phospholipase A2 in drug induced phospholipidosis. Drug Metab Lett. 2007;1(1):49-53.
  • Shayman JA. ELIGLUSTAT TARTRATE: Glucosylceramide Synthase Inhibitor Treatment of Type 1 Gaucher Disease. Drugs Future. 2010;35(8):613-20.
  • Shayman JA, Kelly R, Kollmeyer J, He Y, and Abe A. Group XV phospholipase A(2), a lysosomal phospholipase A(2). Prog Lipid Res. 2011;50(1):1-13.
  • Glukhova A, Hinkovska-Galcheva V, Kelly R, Abe A, Shayman JA, and Tesmer JJ. Structure and function of lysosomal phospholipase A2 and lecithin:cholesterol acyltransferase. Nat Commun. 2015;6:6250.
  • Hinkovska-Galcheva V, Treadwell T, Shillingford JM, Lee A, Abe A, Tesmer JJG, et al. Inhibition of lysosomal phospholipase A2 predicts drug-induced phospholipidosis. J Lipid Res. 2021;62:100089.
  • Wilson MW, Shu L, Hinkovska-Galcheva V, Jin Y, Rajeswaran W, Abe A, et al. Optimization of Eliglustat-Based Glucosylceramide Synthase Inhibitors as Substrate Reduction Therapy for Gaucher Disease Type 3. ACS Chem Neurosci. 2020;11(20):3464-73.

References[edit]

  1. ^ a b "James A. Shayman, M.D. | Pharmacology | Michigan Medicine | University of Michigan".
  2. ^ a b "Dr. James A. Shayman, MD - Ann Arbor, MI - Nephrologist - US News Doctors".
  3. ^ "James Shayman". scholar.google.com.
  4. ^ "JASN Editorial Board: Journal of the American Society of Nephrology". journals.lww.com.
  5. ^ a b c "James A. Shayman, Professor - eMedEvents". www.emedevents.com.
  6. ^ "James Shayman, MD". Division of Nephrology.
  7. ^ "Amino ceramide-like compounds and therapeutic methods of use".
  8. ^ "Pyridine inhibitors of glucosylceramide synthase and therapeutic methods using the same".
  9. ^ "Improved Inhibitors of Glucosylceramide Synthase1 - The Journal of Biochemistry - Oxford Academic".
  10. ^ Abe, Akira; Gregory, Susan; Lee, Lihsueh; Killen, Paul D.; Brady, Roscoe O.; Kulkarni, Ashok; Shayman, James A. (June 1, 2000). "Reduction of globotriaosylceramide in Fabry disease mice by substrate deprivation". The Journal of Clinical Investigation. 105 (11): 1563–1571. doi:10.1172/JCI9711. PMC 300859. PMID 10841515 – via www.jci.org.
  11. ^ Marshall, John; McEachern, Kerry Anne; Chuang, Wei-Lien; Hutto, Elizabeth; Siegel, Craig S.; Shayman, James A.; Grabowski, Greg A.; Scheule, Ronald K.; Copeland, Diane P.; Cheng, Seng H. (June 1, 2010). "Improved management of lysosomal glucosylceramide levels in a mouse model of type 1 Gaucher disease using enzyme and substrate reduction therapy". Journal of Inherited Metabolic Disease. 33 (3): 281–289. doi:10.1007/s10545-010-9072-z. PMC 3683842. PMID 20336375 – via Springer Link.
  12. ^ Shayman, J.A. (August 1, 2010). "ELIGLUSTAT TARTRATE: Glucosylceramide Synthase Inhibitor Treatment of Type 1 Gaucher Disease". Drugs of the Future. 35 (8): 613–620. doi:10.1358/dof.2010.35.8.1505566. PMC 3340614. PMID 22563139.
  13. ^ Shayman, James A. (October 23, 2013). "The Design and Clinical Development of Inhibitors of Glycosphingolipid Synthesis: Will Invention Be the Mother of Necessity?". Transactions of the American Clinical and Climatological Association. 124: 46–60. PMC 3715929. PMID 23874009.
  14. ^ "Cell Cycle Arrest Induced by an Inhibitor of Glucosylceramide Synthase - Journal of Biological Chemistry".
  15. ^ Zador, I. Z.; Deshmukh, G. D.; Kunkel, R.; Johnson, K.; Radin, N. S.; Shayman, J. A. (March 1, 1993). "A role for glycosphingolipid accumulation in the renal hypertrophy of streptozotocin-induced diabetes mellitus". The Journal of Clinical Investigation. 91 (3): 797–803. doi:10.1172/JCI116299. PMC 288030. PMID 8450061 – via www.jci.org.
  16. ^ Natoli, Thomas A.; Smith, Laurie A.; Rogers, Kelly A.; Wang, Bing; Komarnitsky, Svetlana; Budman, Yeva; Belenky, Alexei; Bukanov, Nikolay O.; Dackowski, William R.; Husson, Hervé; Russo, Ryan J.; Shayman, James A.; Ledbetter, Steven R.; Leonard, John P.; Ibraghimov-Beskrovnaya, Oxana (July 23, 2010). "Inhibition of glucosylceramide accumulation results in effective blockade of polycystic kidney disease in mouse models". Nature Medicine. 16 (7): 788–792. doi:10.1038/nm.2171. PMC 3660226. PMID 20562878.
  17. ^ Wilson, Michael W.; Shu, Liming; Hinkovska-Galcheva, Vania; Jin, Yafei; Rajeswaran, Walajapet; Abe, Akira; Zhao, Ting; Luo, Ruijuan; Wang, Lu; Wen, Bo; Liou, Benjamin; Fannin, Venette; Sun, Duxin; Sun, Ying; Shayman, James A.; Larsen, Scott D. (October 21, 2020). "Optimization of Eliglustat-Based Glucosylceramide Synthase Inhibitors as Substrate Reduction Therapy for Gaucher Disease Type 3". ACS Chemical Neuroscience. 11 (20): 3464–3473. doi:10.1021/acschemneuro.0c00558. PMC 7919060. PMID 33035424.
  18. ^ Arthur, Julian R.; Wilson, Michael W.; Larsen, Scott D.; Rockwell, Hannah E.; Shayman, James A.; Seyfried, Thomas N. (April 1, 2013). "Ethylenedioxy-PIP2 Oxalate Reduces Ganglioside Storage in Juvenile Sandhoff Disease Mice". Neurochemical Research. 38 (4): 866–875. doi:10.1007/s11064-013-0992-5. PMC 6554746. PMID 23417430 – via Springer Link.
  19. ^ "Property-based design of a glucosylceramide synthase inhibitor that reduces glucosylceramide in the brain - Journal of Lipid Research".
  20. ^ Kang, Justin J.; Kaissarian, Nayiri M.; Desch, Karl C.; Kelly, Robert J.; Shu, Liming; Bodary, Peter F.; Shayman, James A. (January 1, 2019). "α-galactosidase A deficiency promotes von Willebrand factor secretion in models of Fabry disease". Kidney International. 95 (1): 149–159. doi:10.1016/j.kint.2018.08.033. PMC 6320285. PMID 30470436.
  21. ^ Shu, Liming; Park, James L.; Byun, Jaeman; Pennathur, Subramaniam; Kollmeyer, Jessica; Shayman, James A. (September 23, 2009). "Decreased Nitric Oxide Bioavailability in a Mouse Model of Fabry Disease". Journal of the American Society of Nephrology. 20 (9): 1975–1985. doi:10.1681/ASN.2008111190. PMC 2736776. PMID 19628671.
  22. ^ Shu, Liming; Vivekanandan-Giri, Anuradha; Pennathur, Subramaniam; Smid, Bouwien E.; Aerts, Johannes M. F. G.; Hollak, Carla E. M.; Shayman, James A. (July 1, 2014). "Establishing 3-nitrotyrosine as a biomarker for the vasculopathy of Fabry disease". Kidney International. 86 (1): 58–66. doi:10.1038/ki.2013.520. PMC 4077934. PMID 24402087.
  23. ^ Kang, Justin J.; Shu, Liming; Park, James L.; Shayman, James A.; Bodary, Peter F. (January 15, 2014). "Endothelial nitric oxide synthase uncoupling and microvascular dysfunction in the mesentery of mice deficient in α-galactosidase A". American Journal of Physiology-Gastrointestinal and Liver Physiology. 306 (2): G140–G146. doi:10.1152/ajpgi.00185.2013. PMC 3920075. PMID 24232002.
  24. ^ Hiraoka, Miki; Abe, Akira; Lu, Ye; Yang, Kui; Han, Xianlin; Gross, Richard W.; Shayman, James A. (August 1, 2006). "Lysosomal Phospholipase A2 and Phospholipidosis". Molecular and Cellular Biology. 26 (16): 6139–6148. doi:10.1128/MCB.00627-06. PMC 1592808. PMID 16880524.
  25. ^ "Preferential hydrolysis of truncated oxidized glycerophospholipids by lysosomal phospholipase A2 - Journal of Lipid Research".
  26. ^ Hinkovska-Galcheva, Vania; Treadwell, Taylour; Shillingford, Jonathan M.; Lee, Angela; Abe, Akira; Tesmer, John J.G.; Shayman, James A. (June 1, 2021). "Inhibition of lysosomal phospholipase A2 predicts drug-induced phospholipidosis". Journal of Lipid Research. 62: 100089. doi:10.1016/j.jlr.2021.100089. PMC 8243516. PMID 34087196.
  27. ^ "Shayman named 2016 Distinguished University Innovator | The University Record". record.umich.edu.
Retrieved from "https://en.wikipedia.org/w/index.php?title=James_A._Shayman&oldid=1207981516"