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Jessica Beers

Education:

  • Postdoctoral Fellowship, University of Washington School of Pharmacy
  • Doctor of Philosophy (PhD) in Pharmaceutical Sciences, University of North Carolina at Chapel Hill
  • Doctor of Pharmacy (PharmD), Lipscomb University College of Pharmacy

Biography:
Dr. Beers is an assistant professor in the Department of Pharmacy at the University of Washington. Dr. Beers is passionate about drug safety in understudied populations, and her past research has focused on precision medicine, drug-induced liver injury, and using in vitro systems to predict drug metabolism and toxicity. Dr. Beers’ current work combines basic and translational research to investigate drug metabolism and disposition in pregnancy and lactation.

Publications: NIH

Jingjing Yu

Education

  • PhD Degree in Biology,Rensselaer Polytechnic Institute
  • MS Degree in Biology,Rensselaer Polytechnic Institute
  • MS Degree in Psychology,Peking University
  • MD in Preventive Medicine,Peking University

Research Interests

  • Drug disposition and mechanism of PK-based drug interaction
  • Drug-Drug interaction assessment and safety evaluation during drug development
  • Translational research in drug interaction risk prediction, clinical relevance evaluation, and risk management
  • Natural product-Drug interaction evaluation framework

Biography

Dr. Yu received her MD degree in Preventive Medicine and MS degree in Psychology from Peking University (Beijing, China). She obtained her MS degree (2005) and PhD degree in Biology (2007) from Rensselaer Polytechnic Institute (Troy, NY) and then continued her post-doctoral training at Cerep (now Eurofins) followed by UW Medicine. In 2013, Dr. Yu joined UW Drug Interaction Solutions as a Research Scientist and Project Manager. Her role and responsibility have increasingly expanded to manage and supervise the Drug Interaction Database content curation process and the database subscription. In 2019, she was promoted to Associate Director of the program. In July 2020, Dr. Yu joined the faculty of the Department of Pharmaceutics as a Clinical Associate Professor. Dr. Yu’s main research interests relate to drug-drug interaction assessment and safety evaluation of drugs and natural products, especially in drug interaction risk prediction, clinical relevance evaluation, and management.

Selected Publications

https://pubmed.ncbi.nlm.nih.gov/?term=(Yu,+Jingjing%5BAuthor+-+Full%5D)+AND+University+of+Washington%5BAffiliation%5D

 

Lauren Cirrincione

Education

  • Doctor of Pharmacy (PharmD), University of Pittsburgh
  • Master of Public Health (MPH), University of Nebraska Medical Center

Courses Taught

  • PHRMCY 535: Pharmacotherapeutics V

Biography

Dr. Cirrincione is an Associate Professor in the Department of Pharmacy at the University of Washington in Seattle, Washington, USA. Dr. Cirrincione’s research program addresses mechanisms of hormone-mediated drug interactions, focusing on clinical, translational pharmacology in transgender medicine. Dr. Cirrincione holds a Doctor of Pharmacy degree from the University of Pittsburgh School of Pharmacy, Pittsburgh, Pennsylvania, USA, and a Master of Public Health in epidemiology from the University of Nebraska Medical Center, Omaha, Nebraska, USA. Dr. Cirrincione completed a clinical pharmacology fellowship in HIV at the University of Nebraska Medical Center, Omaha, Nebraska, USA.

Selected Publications

https://www.ncbi.nlm.nih.gov/myncbi/lauren.cirrincione.1/bibliography/public/

Catherine Yeung

Education

  • PharmD (University of Michigan)
  • PhD, Medicinal Chemistry (University of Washington)
  • MPH, Epidemiology (University of Washington)

Research Interests

  • Optimizing medication use in patients with Chronic Kidney Disease
  • Microfluidic models of kidney function in health and disease
  • Effects of uremia on drug transport and pharmacokinetics
  • Effects of microgravity on kidney structure and function

Courses Taught

  • PHARM 560
  • PHARM 579
  • PHARM 301
  • PCEUT 586
  • PCEUT 506
  • PHARBE 522

Biography

Dr. Yeung’s research includes both basic science and translational studies, and spans from the determination of molecular mechanisms of altered drug metabolism using 3-dimensional cell culture techniques to the evaluation of the effect of drugs and nutritional supplements on health outcomes in patients receiving hemodialysis. She is a key investigator in the development of a “kidney on a chip” microphysiological system that can be used in preclinical drug development.

Selected Publications

  • Kidneys on Chips: Emerging Technology for Preclinical Drug Development (PMID: 30274990)
  • Human liver-kidney model elucidates the mechanisms of aristolochic acid nephrotoxicity (PMID: 29202460)
  • Does Secretory Clearance Follow Glomerular Filtration Rate in Chronic Kidney Diseases? Reconsidering the Intact Nephron Hypothesis (PMID: 28675584)
  • Effects of chronic kidney disease and uremia on hepatic drug metabolism and transport (PMID: 24132209)
  • Development of a microphysiological model of human kidney proximal tubule function (PMID: 27521113)

H. Steve White

Education:

  • BSci, Pharmacy,
  • MS, Pharmacology
  • PhD, Pharmacology

Courses Taught:

  • Pharm 531

Research Interests:

  • Early discovery of Anti-seizure drugs
  • Animal seizure and epilepsy models for drug discovery
  • Pharmaco-resistant epilepsy
  • Impact of adherence on seizure control
  • comorbidities of epilepsy
  • Prevention and disease modification of epilepsy
  • Role of the community pharmacist in the chronic management of the patient with epilepsy

Biography:

H. Steve White, RpH, Ph.D, earned his baccalaureate degree in Pharmacy and a M.S. in Pharmacology at Idaho State University. He earned his Ph.D. in Pharmacology at the University of Utah where he rose through the academic ranks after joining the College of Pharmacy faculty in 1986.

Before joining the University of Washington School of Pharmacy as Chair of the Department of Pharmacy, White was the principal investigator and scientific director of the NIH-sponsored Anticonvulsant Drug Development (ADD) Program, established in 1975 to identify novel anticonvulsant drugs using established animal seizure and epilepsy models.

White’s research is focused on understanding the factors that contribute to the initiation, propagation, and amelioration of seizure activity.

White has been the recipient of significant research funding from the National Institute of Neurological Disorders and Stroke (NINDS), National Institutes of Health (NIH), and he and his collaborators have published over 170 original papers pertaining to the mechanism of action and the pharmacology of antiepileptic drugs. In addition to his academic service, he served as Research Director of CURE (Citizen’s United for Research in Epilepsy), the largest non-governmental provider of epilepsy research funding, from November 2011 until October of 2015, where he assisted in the development of strategic programs that advance transformative epilepsy research that may someday lead to a cure or disease modifying therapy for the patient at risk for developing epilepsy. He continues to serve as a Research Advisor to CURE’s team-science initiatives. He has been a co-organizer of two NIH-sponsored workshops on models of refractory epilepsy and epileptogenesis and currently serves on the organizing committee of the biannual Eilat Conferences on Antiepileptic Drug Development. Additionally, White has been actively engaged as a mentor for the next generation of neuroscientists and epilepsy educators and is frequently invited to speak at national and international congresses.

In 2011, White received an Honorary Doctor of Science from The University of Copenhagen Faculty of Pharmaceutical Sciences, Copenhagen, Denmark. In 2014, he was named the 2014 recipient of the Epilepsy Foundation’s Lifetime Accelerator Award, in recognition of his commitment and pioneering contributions to the field of epilepsy and seizures.

White was appointed as the new chair for the Department of Pharmacy in January, 2016.

Selected Publications:

https://www.ncbi.nlm.nih.gov/pubmed/?term=H.+Steve+White

Rheem Totah

Accepting Students to Lab: Yes

Education

  • B.S. (Honors), 1995, Birzeit University, Palestine
  • Masters (Honors), 2000, University of Kansas
  • Ph.D. (Honors), 2002, University of Kansas

Research Interests

  • Prescription drug negative side effects in the heart, skeletal muscle and bone; associated chemical mechanisms for this toxicity
  • Drug-endogenous substrate interactions
  • Pharmacogenetics

Biography

Dr. Totah obtained her bachelor’s degree in chemistry from Birzeit University in Palestine and her master’s and PhD in medicinal chemistry from the University of Kansas. Dr. Totah is currently a professor in the Department of Medicinal Chemistry. Her research is in the area of prescription drug negative side effects especially in the heart, skeletal muscle and bone. She focuses on researching the chemical mechanisms for this toxicity. Her research is important in guiding research towards medicines with fewer side effects and safer use. Research in the Totah lab is broadly centered on drug-endogenous substrate interactions.

Recent Publications

A Rapid and Reliable Absorbance Assay to Identify Drug-Drug Interactions with Thiopurine Drugs. Russell DA, Stafford C, Totah RA. Metabolites. 2024 Dec 19;14(12):715. doi: 10.3390/metabo14120715. PMID: 39728496

Liver CYP4A autophagic-lysosomal degradation (ALD): A major role for the autophagic receptor SQSTM1/p62 through an uncommon target interaction site. He L, Kwon D, Trnka MJ, Liu Y, Yang J, Li K, Totah RA, Johnson EF, Burlingame AL, Correia MA. bioRxiv [Preprint]. 2024 Oct 14:2024.10.14.618315. doi: 10.1101/2024.10.14.618315. PMID: 39464120 Preprint.

A Rapid and Reliable Absorbance Assay to Identify Drug-Drug Interactions with Thiopurine Drugs. Russell DA, Stafford C, Totah RA. Metabolites. 2024 Dec 19;14(12):715.

Editorial: Cytochromes P450, their modulators and metabolites in cardiovascular function and disease. Adebesin AM, Roman RJ, Campbell WB, Seubert JM, Totah RA. Front Pharmacol. 2024 Dec 3;15:1531166.

Liver CYP4A autophagic-lysosomal degradation (ALD): A major role for the autophagic receptor SQSTM1/p62 through an uncommon target interaction site. He L, Kwon D, Trnka MJ, Liu Y, Yang J, Li K, Totah RA, Johnson EF, Burlingame AL, Correia MA. bioRxiv [Preprint]. 2024 Oct 14:2024.10.14.618315.

A Case to Support the Continued Use of Rifampin in Clinical Drug-Drug Interaction Studies. Bercu JP, Ponting DJ, Ripp SL, Dobo KL, Totah RA, Bolleddula J. Clin Pharmacol Ther. 2024 Jul;116(1):34-37.

Investigating the association between CYP2J2 inhibitors and QT prolongation: a literature review. Wiley AM, Yang J, Madhani R, Nath A, Totah RA. Drug Metab Rev. 2024 Mar 20:1-19.

The methyltransferases METTL7A and METTL7B confer resistance to thiol-based histone deacetylase inhibitors. Robey RW, Fitzsimmons CM, Guiblet WM, Frye WJE, González Dalmasy JM, Wang L, Russell DA, Huff LM, Perciaccante AJ, Ali-Rahmani F, Lipsey CC, Wade HM, Mitchell AV, Maligireddy SS, Terrero D, Butcher D, Edmondson EF, Jenkins LM, Nikitina T, Zhurkin VB, Tiwari AK, Piscopio AD, Totah RA, Bates SE, Arda HE, Gottesman MM, Batista PJ. Mol Cancer Ther. 2023 Dec 28.

Cardioprotective mechanisms of cytochrome P450 derived oxylipins from ω-3 and ω-6 PUFAs. Cho C, Aliwarga T, Wiley AM, Totah RA. Adv Pharmacol. 2023;97:201-227.

METTL7A (TMT1A) and METTL7B (TMT1B) are responsible for alkyl S-thiol methyl transferase activity in liver. Russell DA, Chau MK, Shi Y, Levasseur IN, Maldonato BJ, Totah RA. Drug Metab Dispos. 2023 May 3:DMD-AR-2023-001268.

Effects of Pregnancy on Plasma Sphingolipids Using a Metabolomic and Quantitative Analysis Approach. Enthoven LF, Shi Y, Fay E, Kim A, Moreni S, Mao J, Isoherranen N, Totah RA, Hebert MF. Metabolites. 2023 Sep 21;13(9):1026.

CYP2D6 Activity Is Correlated with Changes in Plasma Concentrations of Taurocholic Acid during Pregnancy and Postpartum in CYP2D6 Extensive Metabolizers. Czuba LC, Malhotra K, Enthoven L, Fay EE, Moreni SL, Mao J, Shi Y, Huang W, Totah RA, Isoherranen N, Hebert MF. Drug Metab Dispos. 2023 Nov;51(11):1474-1482.

Cardioprotective mechanisms of cytochrome P450 derived oxylipins from ω-3 and ω-6 PUFAs. Cho C, Aliwarga T, Wiley AM, Totah RA. Adv Pharmacol. 2023;97:201-227.

METTL7A (TMT1A) and METTL7B (TMT1B) Are Responsible for Alkyl S-Thiol Methyl Transferase Activity in Liver. Russell DA, Chau MK, Shi Y, Levasseur IN, Maldonato BJ, Totah RA. Drug Metab Dispos. 2023 Aug;51(8):1024-1034.

Plasma hydrogen sulfide, nitric oxide, and thiocyanate levels are lower during pregnancy compared to postpartum in a cohort of women from the Pacific northwest of the United States. Zeigler MB, Fay EE, Moreni SL, Mao J, Totah RA, Hebert MF. Life Sci. 2023 Jun 1;322:121625.

The Effects of Pregnancy on Amino Acid Levels and Nitrogen Disposition. Enthoven LF, Shi Y, Fay EE, Moreni S, Mao J, Honeyman EM, Smith CK, Whittington D, Brockerhoff SE, Isoherranen N, Totah RA, Hebert MF. Metabolites. 2023 Feb 7;13(2):242.

Cardiac Disease Alters Myocardial Tissue Levels of Epoxyeicosatrienoic Acids and Key Proteins Involved in Their Biosynthesis and Degradation. Aliwarga T, Dinh JC, Heyward S, Prasad B, Gharib SA, Lemaitre RN, Sotoodehnia N, Totah RA. Int J Mol Sci. 2022 Oct 17;23(20):12433.

Selective deuteration of bupropion slows epimerization and reduces metabolism. Shi Y, Dinh J, Pelletier R, Raccor B, Yusuff N, Morgan AJ, Harbeson S, Uttamsingh V, Totah RA. Bioorg Med Chem Lett. 2022 Nov 15;76:129009.

Plasma epoxyeicosatrienoic acids and diabetes-related cardiovascular disease: The cardiovascular health study. Lemaitre RN, Jensen PN, Zeigler M, Fretts AM, Umans JG, Howard BV, Sitlani CM, McKnight B, Gharib SA, King IB, Siscovick DS, Psaty BM, Sotoodehnia N, Totah RA. EBioMedicine. 2022 Sep;83:104189.

Reductions in Hydrogen Sulfide and Changes in Mitochondrial Quality Control Proteins Are Evident in the Early Phases of the Corneally Kindled Mouse Model of Epilepsy. Cho C, Zeigler M, Mizuno S, Morrison RS, Totah RA, Barker-Haliski M. Int J Mol Sci. 2022 Jan 27;23(3):1434.

Future of Biotransformation Science in the Pharmaceutical Industry. Kramlinger VM, Dalvie D, Heck CJS, Kalgutkar AS, O’Neill J, Su D, Teitelbaum AM, Totah RA. Drug Metab Dispos. 2022 Mar;50(3):258-267.

Full PubMed Listing

Kenneth Thummel

Education

  • B.S., Chemistry
  • Ph.D., Pharmaceutical Sciences

Research Interests

  • Drug metabolism kinetics
  • Intestinal first-pass metabolism
  • Mechanisms of inter-individual variability in metabolic drug clearance and drug response
  • Pharmacogenetics
  • Fat soluble vitamins and regulation of DMETs

Courses Taught

  • PCEUT 502
  • PCEUT 506
  • PCEUT 510
  • PCEUT 513
  • PCEUT 534
  • PCEUT 583
  • PCEUT 586
  • MEDCH 527

Biography

Kenneth Thummel received his Ph.D. in Pharmaceutical Science from the University of Washington in 1987 and completed a post-doctoral fellowship in Pharmacology at the University of Connecticut Health Science Center. In 1989, he was appointed to the University of Washington School of Pharmacy faculty, promoted to the rank of Professor in 2001 and was Chairman of the Department of Pharmaceutics between 2006 – 2019. He currently holds the title of Professor of Pharmaceutics and is an Adjunct Professor in the UW Department of Environmental and Occupational Health Sciences. Dr. Thummel’s research interests include the elucidation of genetic, hormonal and environmental factors that contribute to interindividual differences in xenobiotic biotransformation, in particular, intestinal cytochrome P450 3A-mediated first-pass drug metabolism, as well as gene x diet modifiers of drug response in Alaska Native and American Indian people. Dr. Thummel is a Fellow of the American Association for the Advancement of Science and the American Association of Pharmaceutical Scientists, and the recipient of the Rawls-Palmer Progress in Medicine Award from ASCPT. He is a Past-President of the American Society for Pharmacology and Experimental Therapeutics.

Selected Publications

https://www.ncbi.nlm.nih.gov/pubmed/?term=Thummel+K

Isabelle Ragueneau-Majlessi

Education

  • MD, University of Paris VI
  • Master in Biomedical Regulatory Affairs, University of Washington

Research interests

  • Mechanisms of PK-based drug interactions
  • Regulatory framework of drug interactions assessment
  • Clinical relevance and risk management of drug interactions

Biography

Dr. Ragueneau is co-author of the DIDB and e-PKGene applications (https://www.druginteractionsolutions.org/) and Director of UW Drug Interaction Solutions. She received her medical degree from St Antoine University in Paris, France, and specialized in Clinical Pharmacology. Prior to moving to the US, Dr. Ragueneau designed and supervised clinical studies in the private sector and in academia for over 6 years. She started working at the University of Washington in 1999, as a Research Associate, then Principal Research Scientist and Project Manager for the Drug Interaction Database. In November 2009, Dr. Ragueneau joined the faculty of the Department of Pharmaceutics as Clinical Associate Professor and was promoted to full Professor in 2014. Dr. Ragueneau has published in the areas of drug-drug interactions (DDIs), drug disposition and clinical pharmacology. She is interested in the regulatory framework of DDI assessment and the clinical relevance of drug interactions. Dr. Ragueneau graduated from the University of Washington’s Master’s Degree Program in Biomedical Regulatory Affairs in 2010. In 2015, she was named a UW CoMotion Presidential Innovation Fellow.

Selected Publications

PubMed link: https://www.ncbi.nlm.nih.gov/pubmed?term=ragueneau-majlessi[Author]%20OR%20ragueneau%20i[Author]

Yvonne Lin

Accepting Students to Lab: Yes

Education

  • BA in Biophysics, University of California at Berkeley
  • PhD in Pharmaceutical Sciences, University of Washington

Research Interests:

  • Pharmacokinetics/pharmacogenomics
  • Natural products research
  • Regulation of drug metabolizing enzymes in children and pregnant women

Courses Taught

  • PHARBE 506
  • PHARBE 510
  • PCEUT 507
  • PCEUT 537

Biography

Dr. Lin is an Assistant Dean for Academic Affairs and Associate Professor in the Department of Pharmaceutics. She received her BA in Biophysics from the University of California at Berkeley and her PhD in Pharmaceutical Sciences from the University of Washington, and completed a postdoctoral fellowship at St. Jude Children’s Research Hospital.

Her research interests include: natural product-drug interactions, regulation of drug metabolizing enzymes in children and in pregnancy, and using metabolomics to discover endogenous biomarkers of drug metabolism and transport.

Selected Publications

https://www.ncbi.nlm.nih.gov/myncbi/yvonne.lin.1/bibliography/public/

Kelly Lee

Accepting Students to Lab: Yes

Education

  • AB (Honors), Harvard University
  • PhD, Johns Hopkins University

Research Interests

  • HIV, Influenza A virus
  • Biophysical, structural, and biochemical techniques including X-ray scattering, cryo-electron microscopy, hydrogen/deuterium-exchange mass spectrometry, and fluorescence microscopy to understand the function of viral machinery

Biography

Our lab uses complementary structural and biophysical methods to characterize the conformational changes viruses carry out in order to invade host cells. We focus on the transitions and the critical functional states that often are too transient or dynamic to characterize by classical structural methods. Understanding these events is essential to understanding mechanisms of cell entry, for understanding the activity of neutralizing antibodies, and also for developing novel antivirals that can target the virus prior to infection. Our core expertise is in using Hydrogen/Deuterium-Exchange Mass Spectrometry (HDX-MS), cryo-electron microscopy (cryo-EM) and small-angle X-ray scattering (SAXS) to monitor conformational change of protein complexes and viruses. An NIH K99/R00 Career Award supported my transition to studying influenza virus with techniques such as cryo-electron tomography and SAXS. Current projects apply cryo-ET, SAXS, and HDX-MS to dissect the spring-loaded membrane fusion mechanism of influenza virus hemagglutinin (HA) and HIV Env.

For example, in recent studies using cryo-ET and HDX-MS, for the first time we have been able to visualize the nature of fusion protein-mediated membrane remodeling and to determine the sequence of events in whole viruses and isolated fusion proteins that are needed to produce efficient fusion.

With the support of a Center for AIDS Research Creative and Novel Ideas in HIV Research (CNIHR) award for new investigators and with Gates Foundation support, my lab is working with Shiu-Lok Hu’s group (Pharmaceutics) to investigate the structural basis for antigenicity and immunogenicity of HIV Env glycoproteins. In addition, we have been able to characterize isolate-specific structural differences and their impact on antigenicity of Env; these effects are difficult to study by conventional approaches. Our biophysical approaches have also enabled us to analyze CD4 receptor, entry inhibitors, and neutralizing Abs in complex with the native-like HIV Env trimers. In collaboration with Julie Overbaugh’s group at the Fred Hutchinson Cancer Research Center, we are gaining insight into the nature of Env-dependent HIV transmission and the development of neutralizing antibodies in response to infection.

Dr. Lee also holds an adjunct appointment in the UW Microbiology Department and is a member of a number of cross-departmental graduate programs including the Biological Physics Structure and Design Program, the Pathobiology Graduate Program and the Molecular and Cellular Biology Program.

Recent Publications

Visualizing intermediate stages of viral membrane fusion by cryo-electron tomography. Kephart SM, Hom N, Lee KK.Trends Biochem Sci. 2024 Oct;49(10):916-931. doi: 10.1016/j.tibs.2024.06.012. Epub 2024 Jul 24.

Potent neutralization of SARS-CoV-2 variants by RBD nanoparticle and prefusion-stabilized spike immunogens. Miranda MC, Kepl E, Navarro MJ, Chen C, Johnson M, Sprouse KR, Stewart C, Palser A, Valdez A, Pettie D, Sydeman C, Ogohara C, Kraft JC, Pham M, Murphy M, Wrenn S, Fiala B, Ravichandran R, Ellis D, Carter L, Corti D, Kellam P, Lee K, Walls AC, Veesler D, King NP. NPJ Vaccines. 2024 Oct 8;9(1):184.

mRNA-based VP8* nanoparticle vaccines against rotavirus are highly immunogenic in rodents. Roier S, Mangala Prasad V, McNeal MM, Lee KK, Petsch B, Rauch S. NPJ Vaccines. 2023 Dec 22;8(1):190.

Combinatorial immune refocusing within the influenza hemagglutinin RBD improves cross-neutralizing antibody responses Dosey A, Ellis D, Boyoglu-Barnum S, Syeda H, Saunders M, Watson MJ, Kraft JC, Pham MN, Guttman M, Lee KK, Kanekiyo M, King NP. Cell Rep. 2023 Dec 26;42(12):113553.

De novo design of monomeric helical bundles for pH-controlled membrane lysis. Goldbach N, Benna I, Wicky BIM, Croft JT, Carter L, Bera AK, Nguyen H, Kang A, Sankaran B, Yang EC, Lee KK, Baker D. Protein Sci. 2023 Nov;32(11):e4769.

An HIV-1 broadly neutralizing antibody overcomes structural and dynamic variation through highly focused epitope targeting. Hodge EA, Chatterjee A, Chen C, Naika GJ, Laohajaratsang M, Mangala Prasad V, Lee KK. NPJ Viruses 1, 2 (2023). https://doi.org/10.1038/s44298-023-00002-4

Identification of broad, potent antibodies to functionally constrained regions of SARS-CoV-2 spike following a breakthrough infection. Guenthoer J, Lilly M, Starr TN, Dadonaite B, Lovendahl KN, Croft JT, Stoddard CI, Chohan V, Ding S, Ruiz F, Kopp MS, Finzi A, Bloom JD, Chu HY, Lee KK, Overbaugh J. Proc Natl Acad Sci U S A. 2023 Jun 6;120(23):e2220948120.

hACE2-Induced Allosteric Activation in SARS-CoV versus SARS-CoV-2 Spike Assemblies Revealed by Structural Dynamics. Chen C, Zhu R, Hodge EA, Díaz-Salinas MA, Nguyen A, Munro JB, Lee KK. ACS Infect Dis. 2023 Jun 9;9(6):1180-1189.

Structural dynamics reveal subtype-specific activation and inhibition of influenza virus hemagglutinin. Garcia NK, Kephart SM, Benhaim MA, Matsui T, Mileant A, Guttman M, Lee KK. J Biol Chem. 2023 Jun;299(6):104765.

Cytoplasmic Tail Truncation Stabilizes S1-S2 Association and Enhances S Protein Incorporation into SARS-CoV-2 Pseudovirions. Zhang L, Hom N, Ojha A, Lovendahl KN, Mou H, Lee KK, Choe H. J Virol. 2023 Mar 30;97(3):e0165022.

Vaccination with a structure-based stabilized version of malarial antigen Pfs48/45 elicits ultra-potent transmission-blocking antibody responses. McLeod B, Mabrouk MT, Miura K, Ravichandran R, Kephart S, Hailemariam S, Pham TP, Semesi A, Kucharska I, Kundu P, Huang WC, Johnson M, Blackstone A, Pettie D, Murphy M, Kraft JC, Leaf EM, Jiao Y, van de Vegte-Bolmer M, van Gemert GJ, Ramjith J, King CR, MacGill RS, Wu Y, Lee KK, Jore MM, King NP, Lovell JF, Julien JP. Immunity. 2022 Sep 13;55(9):1680-1692.e8.

Visualization of conformational changes and membrane remodeling leading to genome delivery by viral class-II fusion machinery. Mangala Prasad V, Blijleven JS, Smit JM, Lee KK. Nat Commun. 2022 Aug 15;13(1):4772.

Structural dynamics reveal isolate-specific differences at neutralization epitopes on HIV Env.  Hodge EA, Naika GS, Kephart SM, Nguyen A, Zhu R, Benhaim MA, Guo W, Moore JP, Hu SL, Sanders RW, Lee KK. iScience. 2022 May 23;25(6):104449.

Structure-based design of stabilized recombinant influenza neuraminidase tetramers. Ellis D, Lederhofer J, Acton OJ, Tsybovsky Y, Kephart S, Yap C, Gillespie RA, Creanga A, Olshefsky A, Stephens T, Pettie D, Murphy M, Sydeman C, Ahlrichs M, Chan S, Borst AJ, Park YJ, Lee KK, Graham BS, Veesler D, King NP, Kanekiyo M. Nat Commun. 2022 Apr 5;13(1):1825.

Structure-guided changes at the V2 apex of HIV-1 clade C trimer enhance elicitation of autologous neutralizing and broad V1V2-scaffold antibodies. Sahoo A, Hodge EA, LaBranche CC, Styles TM, Shen X, Cheedarla N, Shiferaw A, Ozorowski G, Lee WH, Ward AB, Tomaras GD, Montefiori DC, Irvine DJ, Lee KK, Amara RR. Cell Rep. 2022 Mar 1;38(9):110436.

Cryo-ET of Env on intact HIV virions reveals structural variation and positioning on the Gag lattice. Mangala Prasad V, Leaman DP, Lovendahl KN, Croft JT, Benhaim MA, Hodge EA, Zwick MB, Lee KK. Cell. 2022 Feb 17;185(4):641-653.e17.

Mannose-binding lectin and complement mediate follicular localization and enhanced immunogenicity of diverse protein nanoparticle immunogens. Read BJ, Won L, Kraft JC, Sappington I, Aung A, Wu S, Bals J, Chen C, Lee KK, Lingwood D, King NP, Irvine DJ. Cell Rep. 2022 Jan 11;38(2):110217.

 


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Nina Isoherranen

Accepting Students to Lab: Yes

Education

  • PhD in Pharmaceutical Sciences, Hebrew University of Jerusalem
  • Master of Science in Analytical Chemistry
  • Bachelor of Science in Chemistry, University of Helsinki

Research Interests

  • Metabolism, disposition and biological effects of Vitamin A and Retinoic acid
  • Drug disposition and drug safety during pregnancy
  • Pharmacokinetic modeling and molecular mechanisms of drug-drug interactions

Courses Taught

  • PCEUT532
  • PCEUT506
  • PCEUT502

Biography

Dr. Isoherranen received her bachelor’s degree in chemistry and her master’s degree in Analytical Chemistry in 1998 from the University of Helsinki, Finland. She obtained a PhD from the Hebrew University of Jerusalem in 2003 and continued her training as a post-doctoral fellow with Ken Thummel at the University of Washington. She joined the Department of Pharmaceutics as an Acting Assistant Professor on November 2004.

Dr Isoherranen’s main research interests relate to vitamin A disposition, pharmacokinetic modeling and drug-drug interactions. Her research program includes studies of the role of CYP26 and ALDH1A enzymes in Vitamin A homeostasis, alterations in vitamin A metabolome in obesity and related comorbidities and characterization of how drug and vitamin metabolism change during pregnancy. She has also active research ongoing in the area of pharmacokinetic modeling and PBPK model development relating to predictions of complex drug-drug and disease-drug interactions, and in prediction of clearance changes in different physiological states.

Selected Publications

https://pubmed.ncbi.nlm.nih.gov/term=Isoherranen+N&sort=date&size=20

 

Rene Levy

Accepting New Students: No

Education

  • BS Pharmacy University of Paris, France
  • PhD Pharmaceutical Chemistry UC San Francisco

Research Interests

  • Pharmacokinetics
  • Drug-Drug Interactions
  • Development of new Antiepileptic Drugs

Biography

RENÉ H. LEVY, PhD is Professor Emeritus of Pharmaceutics at the University of Washington in Seattle.
He has served as department chair for 26 years. He has published more than 350 research articles and several books on the treatment of epilepsy.
In 1989, Dr. Levy was named “Ambassador for Epilepsy” by the International Bureau of Epilepsy. In the late 1990s, he co-founded the Eilat Conference on the Development of New Antiepileptic Drugs which is still running on a biennial basis.
In 2007, Dr Levy became “Fellow of the American Association for the Advancement of Science”.
In 2011, Dr. Levy received a “Lifetime Achievement Award from the Epilepsy Foundation”. The foundation’s president and CEO said of Levy: “He is well deserving of this award honoring his career commitment in development of prescription drug therapy for people living with epilepsy.
In 2013, Dr Levy received the William G. Lennox-Cesare T. Lombroso Award, the highest award given by the American Epilepsy Society, in recognition of lifetime accomplishment and contributions related to epilepsy.

Selected Publications

  • Colins C, Levy R, Ragueneau-Majlessi I, Hachad H. Prediction of maximum exposure in poor metabolizers following inhibition of nonpolymorphic pathways. Curr Drug Metab. 2006 Apr;7(3):295-9
  • Levy RH, Collins C. Risk and predictability of drug interactions in the elderly. Int Rev. Neurobiol. 2007;81:235-51.
  • Zhang H, Ragueneau-Majlessi I, Levy RH. Interaction between clopidogrel and proton pump inhibitors: hypothesis to explain multifactorial CYP2C19 inhibition. Drug Metab Lett. 2009 Dec;3(4):287-9.
  • Hachad H, Overby CL, Argon S, Yeung CK, Ragueneau-Majlessi I, Levy RH. e-PKGene: a knowledge-based research tool for analysing the impact of genetics on drug exposure. Hum Genomics. 2011 Jul 1;5(5):506-15.
  • Bialer M, Johannessen SI, Koepp MJ, Levy RH, Perucca E, Tomson T, White HS Progress report on new antiepileptic drugs: A summary of the Fourteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XIV). I. Drugs in preclinical and early clinical development. Epilepsia. 2018 Oct;59(10):1811-1841. doi: 10.1111/epi.14557.
  • Bialer M, Johannessen SI, Koepp MJ, Levy RH, Perucca E, Tomson T, White HS. Progress report on new antiepileptic drugs: A summary of the Fourteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XIV). II. Drugs in more advanced clinical development. Epilepsia. 2018 Oct;59(10):1842-1866. doi: 10.1111/epi.14555. Erratum in: Epilepsia. 2019 Jan;60(1):187.
  • Levy RH, Ragueneau-Majlessi I. Past, Present, and Future of Drug-Drug Interactions. Clin Pharmacol Ther. 2019 Feb 17. doi: 10.1002/cpt.1349.

Rodney JY Ho

Accepting Students to Lab: Yes

Websites

TLC-ART Program

WE-REACH Center

Education

  • PhD, University of Tennessee
  • Bachelor of Science, University of California
  • Post-Doctoral Fellow, Stanford University Internal Medicine

Research Interests

Dr. Ho is known for bio-nanotechnology bio-pharmaceutical research and education that enable transformation of basic biomedical discovery into therapeutics. In addition to innovations in targeted and drug combination synchronous delivery, his research focuses on biology and comprehensive approach to treatments of cancer and infectious diseases of pandemic potential. Some topics include (1) Systems approach to drug combination delivery, transport to target tissues and cells related to disease state intended to improve efficacy and safety; (2) Targeted and Long-acting Combination Anti-Retroviral Therapies and organized TLC-ART program intended for maximizing therapeutic impacts on adults and children (3) Drug and lipid or biomaterial interaction studies that enable the engineering and development of long acting and targeted systems that enhance drug potency and safety.

Biography

Dr. Ho is a professor and presidential entrepreneurial fellow of the University of Washington, and holds appointments at the Fred Hutchinson Cancer Research Center. Professor Ho is the founding Executive Director of the Washington Entrepreneurial Research Evaluation and Commercialization Hub (WE-REACH, a NIH designated National Hub). He has served in a number of leadership roles including Assoc Dean for Research and New Initiatives. His current TLC-ART program, built on a collaborative basic and translational research team composed of scientists, physicians, students and post-doc, focuses on developing targeted, drug-combination and long-acting therapeutics for HIV/AIDS and cancer.  Ho is a distinguished leader in pharmaceutical sciences and systems pharmacology with a proven track record of innovation in long-acting and targeted drug combination therapies for AIDS and Cancer. He serves on a number of national and international initiatives relating to Cancer and HIV therapeutics including LEAP leadership team to facilitate development of long-acting therapies for NIH and WHO’s Unitaid. He is an expert on pharmacology and systems approaches to drug targeting and long-acting therapy. His research aims to improve the therapeutic efficacy and safety of viral and cancer drugs, medical diagnostic agents and vaccines. He is an elected member of National Academy of Innovators, elected fellow of the American Association for the Advancement of Science (AAAS) and the American Association of Pharmaceutical Scientists (AAPS). He studies the relationships between drug target distribution and disease development in cancer, AIDS, and neurological disorders. Building on this understanding, he has developed a systems approach to drug delivery and targeting. He is known for his expertise in bio-therapeutics, lipid-drug and -protein interactions, liposomes, drug-combination nanoparticles, pharmacokinetics, and the interplay between tissue targets and drug penetration. His research has led to enhanced HIV, cancer, and pain medication potency and safety. In addition, he has served as an editor of the Journal of Pharmaceutical Sciences and the author of “Biotechnology and Biopharmaceuticals: Transforming Proteins and Genes into Drugs.” He has also received top honors including the Paul Dawson Biotechnology life-time achievement award, Volwiler life-time research achievement award and the AAPS Biotechnology Research achievement, one of the AAPS’s highest recognitions.

Selected Publications

PubMed link

Ho RJY. “Warp-Speed Covid-19 Vaccine Development: Beneficiaries of Maturation in Biopharmaceutical Technologies and Public-Private Partnerships. J Pharm Sci. 2021, 110(2):615-618. PMID: 33212162

Bak A, Ho RJY. “Advancing Cell and Gene Therapeutic Products for Health Impact – Progress on Pharmaceutical Research, Development, Manufacturing and Controls.” J Pharm Sci. 2021, 110(5):1869-1870. PMID: 33189694. 

Perazzolo S, Zhu L, Lin W, Nguyen A, Ho RJY. “Systems and Clinical Pharmacology of COVID-19 Therapeutic Candidates: A Clinical and Translational Medicine Perspective.” J Pharm Sci. 2021, 110:1002-1017. PMID: 33248057

Ho RJY, Gibaldi M. “Biotechnology and Biopharmaceuticals: Transforming proteins and genes into drugs,” John Wiley and Sons, N.Y., 2nd edition 2013.

Gao Y, Kraft JC, Yu D, Ho RJY. “Recent developments of nanotherapeutics for targeted and long-acting, combination HIV chemotherapy.” Eur J Pharm Biopharm. 2019 May;138:75-91. PMID: 29678735.

Mu Q, Yu J, McConnachie LA, Kraft JC, Gao Y, Gulati GK, Ho RJY. “Translation of combination nanodrugs into nanomedicines: lessons learned and future outlook.” J Drug Target. 2018 Jun-Jul;26(5-6):435-447. PMID: 29285948.

Perazzolo S, Shen DD, Ho RJY. Physiologically Based Pharmacokinetic Modeling of 3 HIV Drugs in Combination and the Role of Lymphatic System after Subcutaneous Dosing. Part 2: Model for the Drug-combination Nanoparticles.

J Pharm Sci. 2022, 111(3):825-837. PMID: 34673094

Bak A, Friis KP, Wu Y, Ho RJY. “Translating Cell and Gene Biopharmaceutical Products for Health and Market Impact. Product Scaling From Clinical to Marketplace: Lessons Learned and Future Outlook.” J Pharm Sci. 2019 Oct;108(10):3169-3175. PMID: 31150697.

Kraft JC, McConnachie LA, Koehn J, Kinman L, Sun J, Collier AC, Collins C, Shen DD, Ho RJY. “Mechanism-based pharmacokinetic (MBPK) models describe the complex plasma kinetics of three antiretrovirals delivered by a long-acting anti-HIV drug combination nanoparticle formulation.” J Control Release. 2018 Apr 10;275:229-241. PMID: 29432823.

Kraft JC, McConnachie LA, Koehn J, Kinman L, Collins C, Shen DD, Collier AC, Ho RJY. “Long-acting combination anti-HIV drug suspension enhances and sustains higher drug levels in lymph node cells than in blood cells and plasma.” AIDS. 2017 Mar 27;31(6):765-770. PMID: 28099191.

Mu Q, Yu J, Griffin JI, Wu Y, Zhu L, McConnachie LA, Ho RJY. “Novel drug combination nanoparticles exhibit enhanced plasma exposure and dose-responsive effects on eliminating breast cancer lung metastasis.” PLoS One. 2020 Mar 6;15(3):e0228557. PMID: 32142553

Selen A, Müllertz A, Kesisoglou F, Ho RJY, Cook JA, Dickinson PA, Flanagan T.“Integrated Multi-stakeholder Systems Thinking Strategy: Decision-making with Biopharmaceutics Risk Assessment Roadmap (BioRAM) to Optimize Clinical Performance of Drug Products.” AAPS J. 2020 Jul 27;22(5):97. PMID: 32719954

Ho RJY. “Midyear Commentary on Trends in Drug Delivery and Clinical Translational Medicine: Growth in Biosimilar (Complex Injectable Drug Formulation) Products Within Evolving Collaborative Regulatory Interagency (FDA, FTC, and DOJ) Practices and Enforcement.” J Pharm Sci. 2017 Feb;106(2):471-476.

Kraft JC, Treuting PM, Ho RJY. “Indocyanine green nanoparticles undergo selective lymphatic uptake, distribution and retention and enable detailed mapping of lymph vessels, nodes and abnormalities.” J Drug Targeting. 2018 Jun-Jul;26(5-6):494-504. PMID: 29388438.

Perazzolo S, Shireman LM, Koehn J, McConnachie LA, Kraft JC, Shen DD, Ho RJY. “Three HIV Drugs, Atazanavir, Ritonavir, and Tenofovir, Coformulated in Drug-Combination Nanoparticles Exhibit Long-Acting and Lymphocyte-Targeting Properties in Nonhuman Primates.” J Pharm Sci. 2018 Dec;107(12):3153-3162. PMID: 30121315.

Koehn J, Iwamoto JF, Kraft JC, McConnachie LA, Collier AC, Ho RJY. “Extended cell and plasma drug levels after one dose of a three-in-one nanosuspension containing lopinavir, efavirenz, and tenofovir in nonhuman primates.” AIDS. 2018 Nov 13;32(17):2463-2467. PMID:30102655.

McConnachie LA, Kinman LM, Koehn J, Kraft JC, Lane S, Lee W, Collier AC, Ho RJY. “Long-Acting Profile of 4 Drugs in 1 Anti-HIV Nanosuspension in Nonhuman Primates for 5 Weeks After a Single Subcutaneous Injection.” J Pharm Sci. 2018 Jul;107(7):1787-1790. PMID: 29548975.

Kraft JC, McConnachie LA, Koehn J, Kinman L, Collins C, Shen DD, Collier AC, Ho RJY. “Long-acting combination anti-HIV drug suspension enhances and sustains higher drug levels in lymph node cells than in blood cells and plasma”. AIDS. 2017 Mar 27;31(6):765-770.

Kraft JC, Freeling JP, Wang Z, Ho RJY. “Emerging research and clinical development trends of liposome and lipid nanoparticle drug delivery systems.” J Pharm Sci 103:29-52. 2014.

Freeling JP, Koehn J, Shu J, Sun J, Ho RJY. “Long-Acting Three-Drug Combination Anti-HIV Nanoparticles Enhance Drug Exposure in Primate Plasma and Cells within Lymph Nodes and Blood.” AIDS 28: 2625-2631, 2015 (highlighted by an accompanying editorial commentary in AIDS).

 

William Atkins

Accepting Students to Lab: No

Education

  • BS in Chemistry, The College of William and Mary
  • MA in Pharmacology, Harvard University
  • PhD in Biochemistry, The University of Illinois

Research Interests

  • Drug Metabolizing Enzymes
  • Therapeutic Antibodies
  • Protein structure and Function

Courses Taught

  • MEDCH 531
  • MEDCH 501
  • MEDCH 528
  • MEDCH 327
  • MEDCH 527
  • MEDCH 529

Biography

Dr. William M. Atkins earned a Masters Degree in Pharmacology from Harvard University in 1983 and a Ph.D. in Biochemistry from the University of Illinois at Urbana-Champaign in 1988. From 1988-1991 Dr. Atkins performed postdoctoral research in the Department of Chemistry at The Pennsylvania State University, as an NIH Kirschstein Postdoctoral Fellow.

Dr. Akins was the Sidney D. Nelson Professor and Chair of Medicinal Chemistry at The University of Washington from 2016-2025, having been on the faculty there since 1991. He was Graduate Program Director for the Department of Medicinal Chemistry and co-Director of the Analytical Biopharmacy Core. His research  focuses on the enzymology of detoxification enzymes and drug metabolism, with particular emphasis on biophysical mechanisms. Professor Atkins has been awarded NIH grants for research on several enzyme systems including Cytochrome P450s, Glutathione S-transferases, and the P-glycoprotein efflux transporter. Recent research efforts also include characterization of nanoparticles for drug delivery and therapeutic antibody drug conjugates.

Professor Atkins serves on the International Organizing Committee for The Biennial International Conferences on Cytochrome P450’s and the International Microsomes and Drug Oxidations Conference. Dr. Atkins has served on several NIH and NSF Review Panels. He is also a member of the Editorial Boards of Archives in Biochemistry and Biophysics and Environmental Toxicology.

 

Selected Publications

The origins of nonideality exhibited by monoclonal antibodies and Fab fragments in human serum. Larsen HA, Atkins WM, Nath A. Protein Sci. 2023 Dec;32(12):e4812. doi: 10.1002/pro.4812.

Nanodisc-embedded cytochrome P450 P3A4 binds diverse ligands by distributing conformational dynamics to its flexible elements. Paço L, Hackett JC, Atkins WM. J Inorg Biochem. 2023 Jul;244:112211. doi: 10.1016/j.jinorgbio.2023.112211. Epub 2023 Apr 5.

Low molecular weight ligands bind to CYP3A4 via a branched induced fit mechanism: Implications for O2 binding. Redhair M, Nath A, Hackett JC, Atkins WM. Arch Biochem Biophys. 2023 May 1;739:109582. doi: 10.1016/j.abb.2023.109582. Epub 2023 Mar 21.

Reversibility and Low Commitment to Forward Catalysis in the Conjugation of Lipid Alkenals by Glutathione Transferase A4-4. Scian M, Paço L, Murphree TA, Shireman LM, Atkins WM. Biomolecules. 2023 Feb 9;13(2):329. doi: 10.3390/biom13020329.

Long Range Communication between the Drug-Binding Sites and Nucleotide Binding Domains of the Efflux Transporter ABCB1. Clouser AF, Atkins WM. Biochemistry. 2022 Apr 19;61(8):730-740. doi: 10.1021/acs.biochem.2c00056. Epub 2022 Apr 6.

Allan Rettie

Accepting Students to Lab: No

Education

  • PhD in Pharmaceutical Sciences, University of Newcastle-upon-Tyne, England
  • BSc, Heriot-Watt University, Scotland
  • Postdoctoral Fellow, UW

Research Areas

  • Biochemistry of the human CYP2 and CYP4 families of P450s
  • Pharmacogenomics of cardiovascular drugs
  • P450-dependent bioactivation and associated adverse reactions

Biography

Dr. Rettie obtained a PhD in Pharmaceutical Sciences in 1983 from the University of Newcastle-upon-Tyne, England, before moving to Seattle to post-doc with Drs. Mont Juchau and Dr. Bill Trager at the UW in the areas of extra-hepatic drug metabolism and mechanisms of drug-drug interactions. He joined the faculty of the UW School of Pharmacy in 1987 and was Department Chair from 2000-2014.

Dr. Rettie’s research interests have focused mainly on the human P450 enzymes and attempts to understand mechanisms of catalysis, substrate specificity, pharmacogenetic variability and adverse drug reactions related to these monooxygenases. He has published over 190 peer-reviewed papers and held research grants from the National Institutes of Health (NIH) in these topic areas for the last 25 years.

Dr. Rettie has served on the editorial boards of Drug Metabolism and Disposition, Drug Metabolism Reviews, Journal of Pharmacology and Therapeutics, Current Drug Metabolism, Chemico-Biological Interactions and Chemical Research in Toxicology, as well as numerous NIH grant review panels. He has chaired the Scientific Affairs Committee of the International Society for Study of Xenobiotics (ISSX) and is Past Chair of the International Union of Basic and Applied Pharmacology’s Section of Drug Metabolism and Transport. In 2005, Dr. Rettie received the North American Scientific Achievement Award from ISSX for his work on elucidating metabolic and pharmacogenetic mechanisms of adverse reactions to the anticoagulant drug, warfarin, and in 2016 was appointed a Fellow of the Japanese Society for the Study of Xenobiotics.

Research Overview

Metabolism by the cytochrome P450s is the principal means whereby lipid-soluble drugs and compounds foreign to the body are converted to water-soluble derivatives that can be readily excreted. This is a beneficial effect of the enzyme system. However, it is well recognized that P450-mediated bioactivation of drugs and other xenobiotics is an important mechanism of chemical toxicity (Baillie and Rettie, 2011). Moreover, unexpected interruptions in P450 activity, due to genetic variation (Danese et al., 2012) or administration of agents that inhibit P450 activity (McDonald et al., 2015), can cause serious adverse drug reactions and contribute to disease states.

Much of the research in the Rettie laboratory focuses on the biochemistry and pharmacogenetics of the vitamin K cycle with an emphasis on how P450 enzymes interact with components of the cycle to maintain homeostasis. Human CYP2C9, for example, is the primary catalyst of (S)-warfarin metabolism (Daly et al., 2018). This vitamin K antagonist is an anticoagulant drug that is very difficult to dose correctly, and there are many drug-drug and drug-gene interactions associated with its use (Rettie and Tai, 2006).

An important goal for the laboratory is to define sources of inter-individual variability in warfarin dosing that can span a 100-fold range (Cooper et al., 2008). We have shown that common genetic polymorphisms in CYP2C9 decrease warfarin dose requirements by reducing the metabolic clearance of (S)-warfarin, while common polymorphisms in the warfarin target enzyme, VKORC1, affect warfarin dose by changing hepatic concentrations of this critical recycling enzyme (Rieder et al., 2005). We found that CYP4F2 and CYP4F11 are key vitamin K catabolizing enzymes (Edson et al., 2013) and common variation in CYP4F2 at least, affects warfarin dose, likely by modulating hepatic vitamin K concentrations (McDonald et al., 2009). We are currently examining the role of novel genetic variation in determining warfarin response in underserved populations (Henderson et al., 2019).

Other research in the laboratory is concerned with CYP4 enzymes that are potential drug targets because of their critical roles in health and disease (Edson et al., 2013; Johnson et al., 2015). Efforts are ongoing to synthesize chemical inhibitors of specific CYP4-family members to better dissect their physiological roles. CYP4B1 metabolizes a host of pro-toxins, including furans, aromatic amines, and certain fatty acids to reactive intermediates that can damage the cell. In this regard, CYP4B1 is a curious member of the CYP4 family because these enzymes typically have
a restricted substrate specificity that does not extend much beyond endogenous fatty acids. To evaluate the role of CYP4B1 in chemical toxicity, we have also developed a knockout mouse model (Parkinson et al, 2013). Most recently, we identified structural determinants of human CYP4B1 that confer high activity towards 4-ipomeanol (Wiek et al., 2015), and evaluated the substrate specificity of the ‘optimized’ human enzyme (Roellecke et al., 2017).

Our CYP4 research extends to the study of ‘orphan P450s’, like CYP4V2 and CYP4Z1, whose substrate specificity is unknown. We have reported on the fatty acid substrate specificity of CYP4V2 (Nakano et al., 2009) and the enzyme’s distribution in the eye (Nakano et al., 2012). Intriguingly, polymorphisms in CYP4V2 are found in patients suffering from the eye disease Bietti’s Crystalline Dystrophy (BCD). A knockout mouse model for CYP4V2 that recapitulates BCD has been developed in collaboration with the Kelly laboratory that should be of help in ‘deorphanizing’ the enzyme (Lockhart et al., 2014). Finally, the newest project in the Rettie lab concerns CYP4Z1, an unusual CYP that is localized to mammary tissue in humans and is up-regulated in breast cancer. We have expressed the enzyme in yeast and HepG2 cells and reported on the fatty acid metabolite profile of the enzyme (McDonald et al., 2017) and the development of novel, selective chemical inhibitors of CYP4Z1 (Kowalski et al., 2020).

In general, we use genetic re-engineering coupled with conventional protein biochemistry methods for the expression and isolation of CYP2 and CYP4 proteins and mutants of interest from heterologous hosts such as E.coli, insect cells and yeast (Mosher et al., 2008; Roberts et al., 2010). We also make extensive use of mass spectrometry for analyte quantification, including evaluation of structural changes in mutant proteins and lipidomic analysis to probe changes in endogenous metabolism due to CYP4V and CYP2C enzyme polymorphisms. Gene sequencing to discover novel polymorphisms in important pharmacogenes and disease-associated P450s is a continuing focus of the laboratory. Synthetic chemistry comes into play in the preparation of new substrates, inhibitors and metabolites for P450s of interest. Our long-term goals are to understand how structure and function are related for these important P450 enzyme families, and how their dysregulation affects drug response and disease.

Recent Publications

Deep mutational scanning of CYP2C19 in human cells reveals a substrate specificity-abundance tradeoff. Boyle GE, Sitko KA, Galloway JG, Haddox HK, Bianchi AH, Dixon A, Wheelock MK, Vandi AJ, Wang ZR, Thomson RES, Garge RK, Rettie AE, Rubin AF, Geck RC, Gillam EMJ, DeWitt WS, Matsen FA 4th, Fowler DM. Genetics. 2024 Nov 6;228(3):iyae156.

Sodium Dehydroacetate and Dehydroacetic Acid. Cherian P, Bergfeld WF, Belsito DV, Cohen DE, Klaassen CD, Rettie AE, Ross D, Slaga TJ, Snyder PW, Tilton S, Fiume M, Heldreth B. Int J Toxicol. 2024 Oct;43(4_suppl):130-134.

Isobutane, Isopentane, Butane, and Propane. Tucker R, Bergfeld WF, Belsito DV, Cohen DE, Klaassen CD, Rettie AE, Ross D, Slaga TJ, Snyder PW, Tilton S, Fiume M, Heldreth B. Int J Toxicol. 2025 Feb;44(1_suppl):17S-21S.

There and Back Again: A Perspective on 20 Years of CYP4Z1. Kowalski JP, Rettie AE. Drug Metab Dispos. 2024 Apr 11:DMD-MR-2024-001670.

Cytochrome P450 Family 4F2 and 4F11 Haplotype Mapping and Association with Hepatic Gene Expression and Vitamin K Hydroxylation Activity. Alade AN, Claw KG, McDonald MG, Prasad B, Rettie AE, Thummel KE. ACS Pharmacol Transl Sci. 2024 Feb 3;7(3):716-732.

Characterization of Gla proteoforms and non-Gla peptides of gamma carboxylated proteins: Application to quantification of prothrombin proteoforms in human plasma. Singh DK, Basit A, Rettie AE, Alade N, Thummel K, Prasad B. Anal Chim Acta. 2023 Dec 15;1284:341972.

Improved methods for the detection of heme and protoporphyrin IX adducts and quantification of heme B from cytochrome P450 containing systems. Pelletier RD, Rettie AE, Kowalski JP. J Chromatogr B Analyt Technol Biomed Life Sci. 2023 Dec 1;1231:123921.

Experimental pharmacology in precision medicine. Urbaniak A, Thummel KE, Alade AN, Rettie AE, Prasad B, De Nicolò A, Martin JH, Sheppard DN, Jarvis MF. Pharmacol Res Perspect. 2023 Dec;11(6):e01147.

An Integrative Approach to Elucidate Mechanisms Underlying the Pharmacokinetic Goldenseal-Midazolam Interaction: Application of In Vitro Assays and Physiologically Based Pharmacokinetic Models to Understand Clinical Observations. Nguyen JT, Tian DD, Tanna RS, Arian CM, Calamia JC, Rettie AE, Thummel KE, Paine MF. J Pharmacol Exp Ther. 2023 Dec;387(3):252-264.

Translating Kratom-Drug Interactions: From Bedside to Bench and Back.  Tanna RS, Cech NB, Oberlies NH, Rettie AE, Thummel KE, Paine MF. Drug Metab Dispos. 2023 Aug;51(8):923-935.

Clinical Assessment of the Drug Interaction Potential of the Psychotropic Natural Product Kratom. Tanna RS, Nguyen JT, Hadi DL, Layton ME, White JR, Cech NB, Oberlies NH, Rettie AE, Thummel KE, Paine MF. Clin Pharmacol Ther. 2023 Jun;113(6):1315-1325.

Spotlight on CYP4B1. Röder A, Hüsken S, Hutter MC, Rettie AE, Hanenberg H, Wiek C, Girhard M. Int J Mol Sci. 2023 Jan 20;24(3):2038.

A Physiological-Based Pharmacokinetic Model Embedded with a Target-Mediated Drug Disposition Mechanism Can Characterize Single-Dose Warfarin Pharmacokinetic Profiles in Subjects with Various CYP2C9 Genotypes under Different Cotreatments. Cheng S, Flora DR, Rettie AE, Brundage RC, Tracy TS. Drug Metab Dispos. 2023 Feb;51(2):257-267.

Pharmacokinetic Modeling of Warfarin І – Model-based Analysis of Warfarin Enantiomers with a Target Mediated Drug Disposition Model Reveals CYP2C9 Genotype-dependent Drug-drug Interactions of S-Warfarin. Cheng S, Flora DR, Rettie AE, Brundage RC, Tracy TS. Drug Metab Dispos. 2022 Jul 7;50(9):1287-301.

Pharmacokinetic Modeling of Warfarin ІI – Model-based Analysis of Warfarin Metabolites following Warfarin Administered either Alone or Together with Fluconazole or Rifampin. Cheng S, Flora DR, Rettie AE, Brundage RC, Tracy TS. Drug Metab Dispos. 2022 Jul 7;50(9):1302-11.

Clinical Pharmacokinetic Assessment of Kratom (Mitragyna speciosa), a Botanical Product with Opioid-like Effects, in Healthy Adult Participants. Tanna RS, Nguyen JT, Hadi DL, Manwill PK, Flores-Bocanegra L, Layton ME, White JR, Cech NB, Oberlies NH, Rettie AE, Thummel KE, Paine MF. Pharmaceutics. 2022 Mar 11;14(3):620.

Adapting regulatory drug-drug interaction guidance to design clinical pharmacokinetic natural product-drug interaction studies: A NaPDI Center recommended approach. Cox EJ, Rettie AE, Unadkat JD, Thummel KE, McCune JS, Paine MF. Clin Transl Sci. 2022 Feb;15(2):322-329.