Wendy Bollag, PhD, FAHA

Professor of Physiology, VA Research Career Scientist

Dr. Wendy Bollag

Lab Team

Sara Chen, MD

Research Manager

Vivek Choudhary, DVM, PhD

Assistant Research Scientist

Shinjini Spaulding

Graduate Student

Yonghong Luo

Graduate Student

Sam Melnyk

Graduate Student

Purnima Merai, MS

Part-time Research Assistant

Ismail Kaddour-Djebbar

Postdoctoral Fellow

Phone: (706) 721-0698
Fax: (706) 721-7299
Email: wbollag@augusta.edu
Office: CB-1008
Lab: CB-1055

Dr. Bollag's Faculty Profile

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^{Left image: Pictured left to right: Dr. Ismail Kaddour-Djebbar, Lawrence Olala, Dr.
Wendy Bollag, Dr. Vivek Choudhary, Dr. Sara Chen (2016)}^{Right Image: Pictured left to right: Back Row: Dr. Ismail Kaddour-Djebbar, Dr. Vivek Choudhary, Inas Helwa, Lawrence Olala; Front Row: Ying-Ying Tsai, Dr. Wendy Bollag, Purnima Merai, Dr. Sara Chen (2013)}

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Education & Training

Pennsylvania State University, University Park, PA, BS in Biochemistry, 1984

Yale University, New Haven, CT, MPhil (1987) and PhD in Cellular and Molecular Physiology, 1990

Hoffmann-La Roche, Inc., Nutley, NJ, post-doctoral fellowship in Pre-Clinical Dermatologic Research, 1991

Academic Appointments

2009-present: Professor, Department of Physiology and College of Graduate Studies, 51吃瓜黑料曝料, 51吃瓜黑料曝料, GA

2011-present: Adjunct Professor, Department of Oral Biology (Dental College of Georgia), 51吃瓜黑料曝料, 51吃瓜黑料曝料, GA

2009-present: Adjunct Professor, Departments of Cellular Biology and Anatomy, Medicine (Dermatology) and Orthopaedic Surgery, 51吃瓜黑料曝料, 51吃瓜黑料曝料, GA

2011-2016: VA Research Career Scientist, Charlie Norwood VA Medical Center

2004-2009: Professor, Department of Medicine, Medical College of Georgia, 51吃瓜黑料曝料, GA

1999-2004: Associate Professor, Department of Medicine, Medical College of Georgia, 51吃瓜黑料曝料, GA

1993-1999: Assistant Professor, Department of Medicine, Medical College of Georgia, 51吃瓜黑料曝料, GA

1992-1993: Assistant Professor, Department of Biology, Seton Hall University, South Orange, NJ

Research Interests

My research interests lie in understanding the mechanisms by which hormones, growth factors, cytokines and other signaling molecules instruct cells to respond appropriately to perform their functions. My laboratory currently has one project investigating the regulation of keratinocyte growth and differentiation and a second defining the signaling mechanisms regulating aldosterone secretion from the adrenal gland. In the first project in skin, we are defining the role of the signaling enzymes phospholipase D (PLD) in promoting epidermal keratinocyte differentiation and protein kinase D (PKD) in supporting keratinocyte proliferation and survival. Our data suggest that PLD promotes keratinocyte differentiation and inhibits proliferation whereas PKD acts in an opposite fashion. By regulating these processes PLD and PKD may play a role in the development of skin diseases. Our second project investigates the mechanism by which very low-density lipoprotein (VLDL), the levels of which are elevated in obesity, stimulates the production of aldosterone. As a key hormone involved in sodium homeostasis, aldosterone is an important regulator of blood pressure, and abnormalities in its levels can contribute to various cardiovascular pathologies including hypertension. Since obesity is often associated with high blood pressure, our research may provide one mechanism by which excess weight contributes to hypertension.

Current Projects

In keratinocytes we have obtained data to suggest that PLD, in particular PLD2, in combination with the glycerol channel aquaporin-3, functions to produce the novel lipid signaling molecule, phosphatidylglycerol, which is involved in regulating early keratinocyte differentiation. By defining the function of this novel PLD-generated lipid signaling system in early keratinocyte differentiation, our research may identify new targets for therapeutic intervention in skin diseases including non-melanoma skin cancers and psoriasis. One mechanism by which phosphatidylglycerol appears to function is through an ability to inhibit toll-like receptor activation by microbial products (pathogen-associated molecular patterns) and endogenous molecules such as anti-microbial peptides acting as danger- or damage-associated molecular patterns. These anti-microbial peptides are up-regulated in psoriasis, and we recently showed that phosphatidylglycerol can improve skin lesions in a mouse model of psoriasis. A similar aquaporin 3/PLD2/phosphatidylglycerol signaling pathway seems to play a role in corneal epithelial wound healing. Finally, we are also currently investigating the mechanism(s) by which VLDL increases aldosterone production, including possible roles of PLD and PKD, as well as its interaction with other aldosterone agonists such as angiotensin II.

Awards & Accomplishments

51吃瓜黑料曝料 Research Institute Distinguished Researcher Award

2019

Medical College of Georgia Exemplary Teaching Award

2018

Medical College of Georgia Institutional Service Award

2018

Medical College of Georgia Exemplary Teaching Award

2017

VA Research Career Scientist Award

2011-2016

Completed the 51吃瓜黑料曝料 Executive Leadership Excellence course

2014-2015

Outstanding Performance Award, Charlie Norwood VA Medical Center

2008-2015

Distinguished Teaching Award, 51吃瓜黑料曝料, The Graduate School

2013

Distinguished Faculty Award, Basic Research, 51吃瓜黑料曝料, Medical College of Georgia

2012

Selected to attend the Association of American Medical Colleges Mid-Career Women Faculty, Professional Development Seminar in Austin, TX

2012

Nomination and selection as a Fellow of the American Heart Association

2011

Distinguished Research Award, Medical College of Georgia, College of Graduate Studies

2010

Distinguished Service Award, Medical College of Georgia, College of Graduate Studies

2009

Representative Publications

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Choudhary V, S Griffith, X Chen & WB Bollag. Pathogen-associated molecular pattern-induced TLR2 and TLR4 activation increases keratinocyte production of inflammatory mediators and is inhibited by phosphatidylglycerol, Mol. Pharmacol., 97: 324-335, 2020 (e-published ahead of print March 15, 2020).
Yang R, S Chowdhury, V Choudhary, X Chen & WB Bollag. Aquaporin-3 expression induced by histone deacetylase inhibitors is mediated in part by peroxisome proliferator activated receptors (PPARs) in keratinocytes, Exp. Dermatol., 29: 380-386, 2020 (e-published ahead of print January 30, 2020).
Bollag WB, LO Olala, D Xie, X Lu, H Qin, V Choudhary, R Patel, D Bogorad, A Estes & MA Watsky. Dioleoylphosphatidylglycerol accelerates corneal epithelial wound healing. Invest. Ophthalmol. Vis. Sci., 61: 29, 2020.
Choudhary V, R Uarantanawong, R Patel, H Patel, W Bao, B Hartney, E Cohen, X Chen, Q Zhong, CM Isales & WB Bollag. Phosphatidylglycerol inhibits toll-like receptor-mediated inflammation by damage-associated molecular patterns. J. Invest. Dermatol., 139: 868-877, 2019 (e-published ahead of print October 31, 2018). *contributed equally to this work
Tsai Y-Y, WE Rainey, MH Johnson & WB Bollag. VLDL-activated cell signaling pathways that stimulate adrenal cell aldosterone production, Mol. Cell. Endocrinol., 433: 138-146, 2016 (e-published ahead of print, May 21, 2016).
Bollag WB, L Aitkens, J White & KA Hyndman. Aquaporin-3 in the epidermis: More than skin deep. Am. J. Physiol. Cell Physiol., 318: C1144-c1153, 2020 (e-published ahead of print April 8, 2020). (Invited review)
Tsai Y-Y, WE Rainey & WB Bollag. Very low-density lipoprotein (VLDL)-induced signals mediating aldosterone production. J. Endocrinol. 232: R115-R129, 2017 (e-published ahead of print December 2, 2016).

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