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Jacquelyn S. Fetrow

From Wikipedia, the free encyclopedia

Jacquelyn S. Fetrow
15th President, Albright College
Assumed office
2017
Preceded byLex O. McMillan III
Personal details
Born1960 (age 63–64)
Pennsylvania
SpouseBrian A. Kell
Parents
  • Mildred F. Fetrow
  • David E. Fetrow
Alma materAlbright College (BS)
Pennsylvania State University (PhD)
Profession
  • Computational biophysicist
  • Academic administrator
Known forComputational biophysics
Websitewww.albright.edu/about-albright/president/

Jacquelyn S. (Jacque) Fetrow (born 1960) is a computational biologist, college administrator, and the 15th president of Albright College.[1] Previously, she served as Provost, Vice President of Academic Affairs, and Professor of Chemistry at the University of Richmond, in Richmond, Virginia.[2] Prior to that appointment, she served as Dean of the College at Wake Forest University in Winston-Salem, North Carolina.[3] She also co-founded a company, GeneFormatics, for which she served as Director and Chief Scientific Officer for four years.

Early life and education

Fetrow is a native of Camp Hill, Pennsylvania.[4] Her mother, Mildred F. Fetrow, was a public school teacher in the West Shore School District, teaching kindergarten, first grade and second grade for many years.[5] Her father, David E. Fetrow, was a carpenter. He also worked as a truck salesman, real estate salesman, and office manager.

Fetrow attended Camp Hill public schools through twelfth grade, Albright College for her bachelor's degree (Biochemistry), and Penn State College of Medicine for a Ph.D. (Biological Chemistry), which she earned in 1986 working with George D. Rose.[6][7] She did post-doctoral stints at the University of Rochester School of Medicine under the mentorship of Fred Sherman, and at the Whitehead Institute at Massachusetts Institute of Technology under the tutelage of Peter S. Kim.

Career

Fetrow worked at the University at Albany, SUNY, from 1990 to 1998, serving as assistant and then associate professor of biological sciences. She then accepted a position at The Scripps Research Institute. Technology that she helped develop at Scripps served as the foundation for GeneFormatics, Inc., the company that Fetrow co-founded and at which she served as Chief Scientific Officer and Director.[8] In August 2003 she was appointed Reynolds Professor of Computational Biophysics at Wake Forest University in the departments of Physics and Computer Science, and in January 2009 she was appointed as Dean of Wake Forest College. She moved to the University of Richmond to serve as Provost and Vice President of Academic Affairs at the University of Richmond in 2014. In 2017 she was appointed president of her alma mater, Albright College.

Research

Fetrow was the first to describe the non-regular protein structure, omega loop, a structure she identified and studied for her doctoral dissertation (work published under the name Jacquelyn F. Leszczynski).[9] Her early research work involved the experimental analysis of these structures in the protein cytochrome c.[10][11][12]

Later, Fetrow's work turned to the classification of functional sites in protein structures, resulting in Fuzzy Functional Forms[13] and active site profiling.[14] This work formed the foundation for the company she co-founded, GeneFormatics. Subsequent development of the active site profiling technology[15][16] was used to create the Peroxiredoxin Classification Index.[17][18][19] This technology has been used to cluster other superfamilies, including the enolases,[20] peroxiredoxins,[19] cytochrome P450s,[21] and arsenate reductases,[22] into functionally relevant clusters.

Awards and honors

  • Alumni Fellow, Pennsylvania State University College of Medicine, 2015[23]
  • Distinguished Alumnus/a Award, Albright College, October 2010[24]
  • Honorary member, Phi Beta Kappa, Wake Forest University, April 2009
  • Teaching Innovation Award (for Bioinformatics course, developed with David John), Center for Teaching and Learning, Wake Forest University, February 2006
  • Young Alumnus/a Achievement Award, Albright College, May 1997[24]
  • Chancellor's Award for Excellence in Teaching, University at Albany, Spring, 1995 (A SUNY-wide award)
  • President's Award for Excellence in Teaching, University at Albany, Spring, 1995[25]
  • Member, Jacob Albright Society of Scholars (for high academic achievement), Albright College, May 1982
  • NRSA Postdoctoral Fellowship (NIH). January, 1987–January, 1990.

Patents awarded

  • US patent 8841132, Poole, L.B., King, S.B., and Fetrow, J.S., "Method for detecting compounds containing sulfenic acid using a 1,3-cyclohexanedione-based probe", issued September 23, 2014 
  • US patent 8486642, Poole, L.B., King, S.B., and Fetrow, J.S., "Method of synthesizing 1,3-cyclohexadione derived reagents useful for detection or isolation of sulfenic acid-containing compounds", issued July 16, 2013 
  • US patent 7803630, Poole, L.B., King, S.B., and Fetrow, J.S., "Method for Detecting Target Compounds Containing Sulfenic Acids Using New Reagents", issued September 28, 2007 
  • US patent 7294748, Poole, L.B., King, S.B., and Fetrow, J.S., "Sulfenic Acid-Reactive Compounds And Their Methods Of Synthesis", issued November 13, 2007 
  • US patent 6631332, Skolnick, J. and Fetrow, J.S., "Methods and Systems for Predicting Protein Function", issued October 7, 2003 

Selected publications

  • Rosen, MR, Leuthaeuser, JB, Parish, CA, & Fetrow, JS (2020). Isofunctional Clustering and Conformational Analysis of the Arsenate Reductase Superfamily Reveals Nine Distinct Clusters. Biochemistry, 59(44), 4262-4284, doi: 10.1021/acs.biochem.0c00651.[22]
  • Harper AF, Leuthaeuser JB, Babbitt PC, Morris JH, Ferrin TE, Poole LB, Fetrow JS. An Atlas of Peroxiredoxins Created Using an Active Site Profile-Based Approach to Functionally Relevant Clustering of Proteins. PLoS Comput Biol. 2017 Feb 10;13(2):e1005284. doi: 10.1371/journal.pcbi.1005284. eCollection 2017 Feb. PMID: 28187133[19]
  • Gober JG, Rydeen AE, Gibson-O'Grady EJ, Leuthaeuser JB, Fetrow JS, Brustad EM. Mutating a Highly Conserved Residue in Diverse Cytochrome P450s Facilitates Diastereoselective Olefin Cyclopropanation. Chembiochem. 2016 Mar 2;17(5):394-7. doi: 10.1002/cbic.201500624. Epub 2016 Feb 4. PMID: 26690878. PMCID: 5241096.[21]
  • Loeser RF, Olex A, McNulty MA, Carlson CS, Callahan M, Ferguson C, Chou J, Leng X, Fetrow JS. Microarray analysis reveals age-related differences in gene expression during the development of osteoarthritis in mice. Arthritis Rheum. 2012 Mar;64(3):705-17. Epub 2011 Oct 3. doi: 10.1002/art.33388. [Epub ahead of print]
  • Lewis DR, Olex AL, Lundy SR, Turkett WH, Fetrow JS, Muday GK. A kinetic analysis of the auxin transcriptome reveals cell wall remodeling proteins that modulate lateral root development in Arabidopsis. Plant Cell. 2013 Sep;25(9):3329-46. doi: 10.1105/tpc.113.114868. Epub 2013 Sep 17.
  • Nelson KJ, Knutson ST, Soito L, Klomsiri C, Poole LB, Fetrow JS. Analysis of the peroxiredoxin family: using active-site structure and sequence information for global classification and residue analysis. Proteins. 2011 Mar;79(3):947-64. doi: 10.1002/prot.22936. Epub 2010 Dec 22.[14]
  • Salsbury Jr., F.R., Knutson, S.T., Poole, LB, and Fetrow, J.S. Functional Site Profiling and Electrostatic Analysis of Cysteines Modifiable to Cysteine Sulfenic Acid. Protein Sci. 2008 Feb;17(2):299-312.
  • Skolnick, J. and Fetrow, J.S. From genes to structure: novel applications of computational approaches in the genomic era. Trends in Biotech. 2000 Jan;18(1):34-39.
  • Skolnick, J., Fetrow, J.S., Kolinski, A. Structural genomics and its importance for gene function analysis. Nature Biotechnology. 2000 Mar;18(3):283-287.
  • Fetrow, J.S. and Skolnick, J. Method for prediction of protein function from sequence using the sequence-to-structure-to-function paradigm with application to glutaredoxins/thioredoxins and T1 ribonucleases. J. Mol. Biol. 1998 Sep 4;281(5):949-968.[13]
  • Fetrow, J.S. and Godzik, A. Function driven protein evolution: A possible proto-protein for the RNA-binding proteins. Proceedings of Pacific Symposium on Biocomputing (Ed. R.B. Altman, A.K. Dunker, L. Hunter T. Klein). 1998 485-496.
  • Fetrow, J.S. Omega Loops: Nonregular secondary structures significant in protein function and stability. FASEB J. 1995 Jun;9(9):708-717.
  • Leszczynski (Fetrow), J.F. and Rose, G.D. Loops in globular proteins: Identification of a novel category of secondary structure. Science. 1986 Nov 14;234(4778):849-55.[9]

References

  1. ^ "Albright College Names Alumna Jacquelyn S. Fetrow as Its 15th President | Albright College". Albright College. 2016-10-28. Retrieved 2018-03-07.
  2. ^ "University of Richmond News". news.richmond.edu. Retrieved 2018-03-07.
  3. ^ "Dean of the College | Inside Higher Ed". insidehighered.com. Retrieved 2018-03-07.
  4. ^ "Camp Hill native to lead Albright College in 2017". PennLive.com. Retrieved 2018-03-07.
  5. ^ "Mildred F. "Millie" Fetrow's Obituary on Patriot-News". Patriot-News. Retrieved 2018-03-07.
  6. ^ "George D. Rose". Johns Hopkins University.
  7. ^ "New Albright president sworn in | Reading Eagle - NEWS". Reading Eagle. Retrieved 2018-03-07.
  8. ^ "The Business of Biotech". www.albright.edu. Retrieved 2018-03-07.
  9. ^ a b Leszczynski JF, Rose GD (November 1986). "Loops in globular proteins: a novel category of secondary structure". Science. 234 (4778): 849–55. Bibcode:1986Sci...234..849L. doi:10.1126/science.3775366. PMID 3775366.
  10. ^ Fetrow JS, Cardillo TS, Sherman F (1989). "Deletions and replacements of omega loops in yeast iso-1-cytochrome c". Proteins. 6 (4): 372–81. doi:10.1002/prot.340060404. PMID 2560195. S2CID 25525703.
  11. ^ Murphy ME, Fetrow JS, Burton RE, Brayer GD (September 1993). "The structure and function of omega loop A replacements in cytochrome c". Protein Science. 2 (9): 1429–40. doi:10.1002/pro.5560020907. PMC 2142463. PMID 8401228.
  12. ^ Mulligan-Pullyblank P, Spitzer JS, Gilden BM, Fetrow JS (April 1996). "Loop replacement and random mutagenesis of omega-loop D, residues 70-84, in iso-1-cytochrome c". The Journal of Biological Chemistry. 271 (15): 8633–45. doi:10.1074/jbc.271.15.8633. PMID 8621494.
  13. ^ a b Fetrow JS, Skolnick J (September 1998). "Method for prediction of protein function from sequence using the sequence-to-structure-to-function paradigm with application to glutaredoxins/thioredoxins and T1 ribonucleases". Journal of Molecular Biology. 281 (5): 949–68. doi:10.1006/jmbi.1998.1993. PMID 9719646.
  14. ^ a b Cammer SA, Hoffman BT, Speir JA, Canady MA, Nelson MR, Knutson S, Gallina M, Baxter SM, Fetrow JS (November 2003). "Structure-based active site profiles for genome analysis and functional family subclassification". Journal of Molecular Biology. 334 (3): 387–401. doi:10.1016/j.jmb.2003.09.062. PMID 14623182.
  15. ^ Huff RG, Bayram E, Tan H, Knutson ST, Knaggs MH, Richon AB, Santago P, Fetrow JS (November 2005). "Chemical and structural diversity in cyclooxygenase protein active sites". Chemistry & Biodiversity. 2 (11): 1533–52. doi:10.1002/cbdv.200590125. hdl:10339/16028. PMID 17191953. S2CID 25066310.
  16. ^ Fetrow JS (July 2006). Active site profiling to identify protein functional sites in sequences and structures using the Deacon Active Site Profiler (DASP). Vol. Chapter 8. pp. 8.10.1–8.10.16. doi:10.1002/0471250953.bi0810s14. ISBN 978-0471250951. PMID 18428769. {{cite book}}: |journal= ignored (help)
  17. ^ Soito L, Williamson C, Knutson ST, Fetrow JS, Poole LB, Nelson KJ (January 2011). "PREX: PeroxiRedoxin classification indEX, a database of subfamily assignments across the diverse peroxiredoxin family". Nucleic Acids Research. 39 (Database issue): D332–7. doi:10.1093/nar/gkq1060. PMC 3013668. PMID 21036863.
  18. ^ Nelson KJ, Knutson ST, Soito L, Klomsiri C, Poole LB, Fetrow JS (March 2011). "Analysis of the peroxiredoxin family: using active-site structure and sequence information for global classification and residue analysis". Proteins. 79 (3): 947–64. doi:10.1002/prot.22936. PMC 3065352. PMID 21287625.
  19. ^ a b c Harper AF, Leuthaeuser JB, Babbitt PC, Morris JH, Ferrin TE, Poole LB, Fetrow JS (February 2017). "An Atlas of Peroxiredoxins Created Using an Active Site Profile-Based Approach to Functionally Relevant Clustering of Proteins". PLOS Computational Biology. 13 (2): e1005284. Bibcode:2017PLSCB..13E5284H. doi:10.1371/journal.pcbi.1005284. PMC 5302317. PMID 28187133.
  20. ^ Knutson ST, Westwood BM, Leuthaeuser JB, Turner BE, Nguyendac D, Shea G, Kumar K, Hayden JD, Harper AF, Brown SD, Morris JH, Ferrin TE, Babbitt PC, Fetrow JS (April 2017). "An approach to functionally relevant clustering of the protein universe: Active site profile-based clustering of protein structures and sequences". Protein Science. 26 (4): 677–699. doi:10.1002/pro.3112. PMC 5368075. PMID 28054422.
  21. ^ a b Gober JG, Rydeen AE, Gibson-O'Grady EJ, Leuthaeuser JB, Fetrow JS, Brustad EM (March 2, 2016). "Mutating a Highly Conserved Residue in Diverse Cytochrome P450s Facilitates Diastereoselective Olefin Cyclopropanation". ChemBioChem. 17 (5): 394–397. doi:10.1002/cbic.201500624. PMC 5241096. PMID 26690878.
  22. ^ a b Rosen MR, Leuthaeuser JB, Parish CA, Fetrow JS (November 2, 2020). "Isofunctional Clustering and Conformational Analysis of the Arsenate Reductase Superfamily Reveals Nine Distinct Clusters". Biochemistry. 59 (44): 4262–4284. doi:10.1021/acs.biochem.0c00651. PMID 33135415. S2CID 226233138.
  23. ^ "19 Penn Staters honored with Alumni Fellow Award | Penn State University". Retrieved 2018-03-07.
  24. ^ a b "Alumni Awards | Albright College". Albright College. Retrieved 2018-03-07.
  25. ^ "Faculty Awards". www.albany.edu. Retrieved 2018-03-07.
This page was last edited on 20 November 2023, at 16:55
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