Medical Student Research Fellowship for Summer 2006
Mentor: Richard J. Auchus
Department: Internal Medicine/Endocrinology & Metabolism
Room number: Y9.308
Mail Code: 8857
Phone number: 8-6751
E-mail: richard.auchus@UTSouthwestern.edu
Project title: biochemistry, physiology, and genetics of human steroid biosynthesis
Human subjects IRB approved project number (where applicable): 0902-505, 1203-776, 1203-811
Animal subjects IRB approved project number (where applicable): N/A
Project Type (patient-based research, animal-based research, or basic research; this characterization is only to permit a general classification for grouping similar types of projects)
basic research and patient-based research
Brief Description of Project:
Basic:
We are interested in determining the biochemical principles and structural features
that govern how hydroxysteroid dehydrogenases function in living cells as primarily
oxidative or reductive enzymes. This project involves site-directed mutagenesis
and modification of tissue culture conditions to alter the directional preference
of these enzymes in vivo. We then perform detailed in vivo and in vitro enzymology
studies of the altered enzymes to understand why these changes are observed.
Clinical:
Pending funding support, we will be developing liquid chromatography/tandem
mass spectrometry assays for serum mineralocorticoids to define the physiology
and genetics of mineralocorticoid-dependent hypertension, in collaboration with
Ronald Victor in the Hypertension Division and the Dallas Heart Study.
Previous Research Activities or Publications with Medical Students:
Tim C. Lee (now a pediatrics resident at UCLA) worked with me for a year after
graduating college and during the summer after his first year in medical school
(1996-1998). He and I developed our yeast system for studying enzymology of
steroidogenic cytochromes P450 (Auchus et al 1998 J Biol Chem 273:3158-3165;
Lee et al 1999 J Clin Endocrinol Metab 84:2104-2110). Tim received the Academic
Pediatric Society/Society for Pediatric Research (APS/SPR) Student Research
Award in 1999 for this work. Tim was chief resident in pediatrics at UCLA and
is now in private practice.
Kavita Vyas, worked in my lab the summer of 2000, characterizing the biochemistry
of fusion proteins to probe the mechanism of action of cytochrome b5 on CYP17.
Kavita won the award for best poster at the 39th Medical Student Research Forum,
which was presented at the Endocrine Society meeting in June 2001, and she is
now a third-year medical student at Columbia.
Daniel Sherbet, MS3, worked in my lab for 2 summers (2001-2002, characterizing
a mutation in CYP17 that causes isolated 17, 20-lyase deficiency by a novel
mechanism. Daniel's oral presentation at the 40th Medical Student Research Forum
was selected as the best talk of the day. The work was presented at the Endocrine
Society meeting in June, 2002 and published (Sherbet et al J Biol Chem 278:48563-48569).
Daniel spent last year as a medical student research Fellow of the Howard Hughes
Medical Institute studying hydroxysteroid dehydrogenases and will be an Internal
Medicine Resident next year.
Kristen Bruce, studied (-)-progesterone (the enantiomer of progesterone) as
an inhibitor of CYP17 and CYP21 in 2001 and started our work on HSD directionality.
Her work on (-)-progesterone was published (Auchus et al Arch Biochem Biophys
409:134-144). She is now in dental school.
David Stidd, MS3, worked here in 2003. He synthesized deuterium-labeled steroids
to measure kinetic isotope effects for CYP17 and CYP21. David won an award for
best basic science poster at the 42nd Medical Student Research Forum, and he
is back in the lab for a 6 month research elective to finish off his work.
Andrew Brandmeier was a SURF student in 2003. He engineered mutations to change
the directional preference of AKR1C9 (rat liver 3 -hydroxysteroid dehydrogenase).
He is now an MD-PhD student at Indiana University and has a paper in press in
Endocrinology
Siareyah Rambally, MS3, identified a mutation in a patient with 17 -hydroxysteroid
type 3 deficiency in 2003. She also demonstrated that the magnitude of the directional
preference for human 17 -hydroxysteroid type 1 in transfected cells was not
fixed but could be varied by changes in culture medium that alter intracellular
nicotinamide cofactor concentrations.
Neema Chokshi and Sarita Singeetham, MS2s, helped to organize our adrenal vein
sampling serum bank, leading to the submission of an Endocrine Society abstract
about new approaches to the diagnosis and understanding the physiology of primary
aldosteronism. On the side, they sequenced the CYP17 gene from a patient with
17-hydroxylase deficiency and won an award for top clinical science poster at
the 2006 MSRF.
We plan to prepare manuscripts for David, Daniel, Siareyah, Neema, and Sarita
this spring.
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