Bridget Ford

Bridget Ford, Ph.D.

Associate Professor, Biology Office Location: AT&T 310 Phone: (210) 832-2153

Dr. Bridget Ford is an Associate Professor in the Department of Biology at UIW. She obtained her bachelor’s degree at St. Mary’s University in Biological Sciences with a minor in Chemistry. She then went on to earn her Ph.D. in Molecular Medicine at UT Health San Antonio in 2012. She completed her postdoctoral fellowship training at the United States Army Institute of Surgical Research in the Extremity Trauma and Regenerative Medicine task area and at UT Health at San Antonio between the Magnetic Resonance Imaging Division and the Department of Medicine. During this time, Dr. Ford was an Adjunct Professor at St. Mary’s University and taught in the Biological Sciences, Chemistry and Exercise and Sports Science Departments.

Dr. Ford teaches Anatomy and Physiology I and II, General Biology I and Lab for Majors, Cell Biology, and a Special Topics course in Endocrinology at UIW. She loves mentoring undergraduates in the research laboratory where her research focuses on understanding the molecular mechanisms involved in renal cell injury in diabetic kidney disease, with a particular emphasis on oxidative stress pathways.

  • 2001-2005: B.A. Biological Sciences/Chemistry (minor), St. Mary’s University, San Antonio, Texas
  • 2007-2012: Ph.D. Molecular Medicine, University of Texas Health Science Center at San Antonio,San Antonio, Texas
  • 2012 – 2014: Postdoctoral Fellow, Oak Ridge Institute for Science and Education Fellowship Award, United States Army Institute of Surgical Research, Extremity Trauma Research/Regenerative Medicine
  • 2014 – 2017: Postdoctoral Fellow, Institutional T32 National Research Service Award, UT Health Science Center at San Antonio Research Imaging Institute/MRI Division and Department of Medicine/Nephrology Division
  • 2018: Gross Anatomy Instructor, UT Health at San Antonio, Occupational Therapy Doctorate Program
  • 2017 – Present: Adjunct Assistant Professor, UT Health at San Antonio, Medicine Renal Diseases
  • 2017 – 2023: Assistant Professor of Biology, University of the Incarnate Word, Biology Department
  • 2023 – Present: Associate Professor of Biology, University of the Incarnate Word, Biology Department

Peer-Reviewed Journal Articles

  • Eid AA, Gorin Y, Fagg BM, Maalouf R, Barnes JL, Block K, Abboud HE. Mechanisms of podocyte injury in diabetes: role of cytochrome P450 and NADPH oxidases. Diabetes. 58(5):1201-1211, 2009. PMCID: PMC2671039
  • Eid AA, Ford BM, Block K, Kasinath BS, Gorin Y, Choudhury GG, Barnes JL, Abboud HE. AMP-activated protein kinase (AMPK) negatively regulates Nox4-dependent activation of p53 and epithelial cell apoptosis in diabetes. J Biol Chem. 85(48):37503-12, 2010. PMCID: PMC2988355
  • Eid AA, Ford BM, Bhandary B, Cavagliery R, Block K, Barnes JL, Gorin Y, Choudhury GG, Abboud HE. Mammalian target of rapamycin regulates Nox4-mediated podocyte depletion in diabetic renal injury. Diabetes. 62(8):2935-47, 2013. PMCID: PMC3717863
  • Ford BM, Eid AA, Gooz M, Barnes JL, Gorin YC, Abboud HE. ADAM17 mediates Nox4 expression and NADPH oxidase activity in the kidney cortex of OVE26 mice. Am J Physiol Renal Physiol. 305(3):F323-32, 2013. PMCID: PMC3742865
  • Chandra SB, Mohan S, Ford BM, Huang L, Janardhanan P, Deo KS, Muir ER, Duong TQ. Targeted Overexpression of endothelial nitric oxide synthase in endothelial cells improves cerebrovascular reactivity in Ins2 Akita-Type 1 diabetic mice. J Cereb Blood Flow Metab. Accepted October 2015. [Epub ahead of print] PMID: 26661212
  • Chowdhury K, Kumar S, Sharma A, Bhagat M, Kamai A, Ford BM * , Asthana S, Mandal CC. Presence of a consensus DNA motif at nearby DNA sequence of the mutation susceptible CG nucleotides. Gene. 639:85-95, 2018. PMID: 289863
  • Do C, Ford BM*, Lee DY, Tan C, Escobar P, Wagner B. Gadolinium-based contrast agents: Stimulators of myeloid-induced renal fibrosis and major metabolic disruptors. Toxicol Appl Pharmacol, (2019). DOI: 10.1016/j.taap.2019.05.009 PMID: 31082427.
  • Bandyopadhayaya S, Ford BM*, and Mandal CC. Cold-hearted: a case for cold stress in cancer risk. Journal of Clinical Pathology. Submitted March 2019

Selected Abstracts

  • 2018 Penn R **, Ford BM, Smith HA. “Investigation of P-Glycoprotein (PGP) Induction by PGP Substrates to Induce Paclitaxel Resistance in Ovarian Cancer Cells.” 11th Annual UIW Research Week
  • 2018 Ford BM, Wauquier F, Feliers, D, Ma R, Choudhury GG, Barnes JL, Dupuy C, Bae YS, Lee DY, Gorin YC. “Calcium-dependent dual oxidase 2 is a novel mediator of oxidative stress and mesangial cell fibrotic injury in response to angiotensin II: Role of Nox4.” 21st Annual Medicine Research Day; UT Health at San Antonio, May 22, 2018
  • 2018 Aguilar E **, Navarro M ** , Ford BM, Wauquier F , Lee, DY, Gorin, YC . “Novel role of dual oxidase 2 as a mediator of podocyte injury in the diabetic environment.” 2018 SACNAS National Diversity in STEM Conference
  • 2018 Ramirez-Pedroza A **, Martinez A **, Ford BM, Wauquier F, Lee, DY, Gorin YC. “Calcium-dependent dual oxidase 2 is a novel source of reactive oxygen species implicated in glomerular mesangial cell fibrotic response to angiotensin II.” 2018 SACNAS National Diversity in STEM Conference
  • 2019 Abraham SM **, Navarro MM **, Wauquier FM, Lee DY, Gorin YC, Ford BM. “Novel role of dual oxidase 2 as a mediator of podocyte injury in the diabetic environment,” 2019. The FASEB Journal 33 (1_supplement), 567.11-567.11 Experimental Biology Conference, Orlando, FL.
  • 2019 Ramirez-Pedroza A **, Martinez A **, Ford BM, Wauquier F, Lee, DY, Gorin YC. “Calcium-dependent dual oxidase 2 is a novel source of reactive oxygen species implicated in glomerular mesangial cell fibrotic response to angiotensin II,” 2019. The FASEB Journal 33 (1_supplement), 567.13-567.13 Experimental Biology Conference, Orlando, FL.

See a complete list of publications here

Invited Talks

  • 2017 “Novel role of dual oxidase 2 as a mediator of glomerular cell injury in diabetes.” Pathology Research Conference, UT Health San Antonio, Texas
  • 2019 “Role of dual oxidase 2 and NADPH oxidases in diabetic kidney disease." Department of Medicine Research Discussions, UT Health San Antonio, Texas
  • BIOL 1402 General Biology I and Lab for Majors
  • BIOL 2321 Anatomy and Physiology I
  • BIOL 2322 Anatomy and Physiology II
  • BIOL 3311 Cell Biology
  • BIOL 4399 Special Topics: Endocrinology

Diabetic kidney disease, or diabetic nephropathy, is a serious and life-threatening complication of type 1 and type 2 diabetes. Our current understanding of the mechanisms that regulate the initiation and progression of diabetic nephropathy is not sufficient to design effective therapies to prevent or reverse kidney damage. The Ford research laboratory explores mechanisms involved in kidney cell injury in diabetic nephropathy with a specific emphasis on oxidative stress, or cell injury due to the production of damaging compounds called oxygen radicals. One specific area that may be of great importance in designing new therapies for diabetic nephropathy is to identify factors that are implicated in the death of glomerular cells, podocytes and mesangial cells, leading to subsequent loss of kidney function.

Recent undergraduate trainees have mastered mammalian tissue culture and used various molecular methods such as real time PCR, western blotting, immunocytochemistry, ELISAs, and enzyme activity assays to identify factors involved in podocyte and mesangial cell injury using an in vitro model system mimicking the diabetic environment. The overall goal Dr. Ford has for all of her trainees is to apply what they learn in the classroom to ask scientific questions in the quest to become independent and creative thinkers