Amal Kaddoumi, PhD

Research Interest

My research focus is on translational and experimental therapeutics, which includes drug development, the identification of novel therapeutic targets, and translational research aimed at discovering therapies for neurodegenerative diseases, such as Alzheimer’s disease (AD) and cerebral amyloid angiopathy (CAA). My research aims to improve our understanding of how vascular factors contribute to AD and CAA, enabling us to reduce risk and develop treatments that specifically target brain vasculature function.

My research focuses on investigating the following:

the role of the functional blood-brain barrier (BBB) in maintaining brain function and homeostasis
role of the vasculature in clearing brain waste products like amyloid-β
the neurovascular unit that works in concert to maintain a healthy brain
targeting the BBB as a preventive and therapeutic approach for AD and CAA
discovery and development of drugs that target brain vasculature dysfunction in AD and CAA
drugs repurposing for AD and CAA

Current ongoing research projects in my laboratory include:

Role of blood-brain barrier (BBB) in the pathogenesis of AD and CAA:
The blood-brain barrier (BBB) plays a vital role in maintaining the neurovascular unit function and, thus, brain hemostasis. Amyloid-beta (Aβ) accumulation on brain microvessels contributes to the pathogenesis and progression of Aβ vascular pathology related to AD and CAA. Findings from our studies in transgenic mouse models of AD and CAA demonstrated increased BBB leakage and decreased expression of tight junction and transport proteins causing Aβ accumulation, neuroinflammation, and neurodegeneration. My lab produced several publications that support targeting the endothelial cells of the BBB as a preventive and therapeutic approach for AD and related disorders. Based on our findings in this area, my lab is leading multiple research projects to 1) identify therapeutic molecules that target the BBB to enhance its integrity and function, 2) studies on elucidating mechanisms of BBB breakdown, and 3) translational research to test the therapeutic targeting of the BBB as a promising approach to prevent conversion of MCI to AD.
Drug discovery and development for AD and related disorders:
Recently, my research team developed an in vitro BBB model with CAA characteristics to high throughput screen (HTS) thousands of compounds to identify hits that could rectify the impaired cell-based BBB model function and integrity. Among the identified hits, several FDA-approved drugs were recognized, a finding which is significant for their potential repurposing to prevent or treat BBB breakdown caused by Aβ in CAA and AD. Repurposing of FDA-approved drugs for treating AD is an innovative approach because these drugs are well-studied and evaluated and could be taken forward to clinical trials, which is one of our primary goals to accomplish in the near future.
Investigate mechanisms and contributing factors to AD pathology:
We found a link between BBB disruption, neurotoxicity, gangliosides dyshomeostasis, and amyloid production. As the pathology of AD is complex, we demonstrated the importance of combination therapy to tackle multiple targets simultaneously.
Extra-virgin olive oil (EVOO) as a medical food:
EVOO is one of the main elements of the Mediterranean diet. Several studies have suggested that EVOO has several health-promoting effects that could protect from and decrease the risk of AD; however, the mechanism(s) by which EVOO exerts such effect was unknown. Studies from my lab investigated the effect of EVOO consumption on BBB function and Aβ clearance across the BBB. Our findings demonstrated that adding EVOO, and its bioactive component oleocanthal, to mice diet restored the BBB function and reduced amyloid- and tau-related pathologies. This effect was associated with improved cognitive function. To translate preclinical findings to humans, my lab has conducted a pilot clinical trial to test the hypothesis that “EVOO consumption stops or delays mild cognitive impairment (MCI) conversion to AD by restoring the BBB function in humans” (NCT03824197). Findings demonstrated EVOO to improve the BBB function and improve memory in MCI. Based on these results, my laboratory has currently initiated a second clinical trial utilizing a multi-OMICS approach using transcriptomics, lipidomics, and metabolomics to investigate the biomolecular mechanisms underlying the response of healthy individuals with AD family history to EVOO (NCT05929924).
Understanding the role of transporters in AD and related disorders pathology:
Investigate the role of membrane transport proteins in determining drugs and endogenous molecules disposition and their role in neurological diseases, mainly AD and CAA. Investigating and understanding transport proteins is fundamental to facilitate therapeutic development. Transport proteins are widely acknowledged as important determinants governing absorption, clearance, and, in many cases, extent of entry into target organs. There is also a greater appreciation that altered transporter function, whether due to aging, genetic polymorphisms, drug interactions, or environmental factors such as dietary constituents, can result in unexpected adverse effects. Findings from my laboratory demonstrated the vital role of Aβ efflux transport proteins at the BBB in maintaining Aβ brain levels. Thus, understanding transporters’ role in regulating Aβ brain levels is essential not only for understanding the basis for Aβ fluxes from the brain but also could potentially serve as a basis for developing novel therapeutics that target the BBB function and integrity.
Pharmacokinetic modeling and drug transport/metabolism for drug discovery and development: We also perform in silico prediction of drug pharmacokinetics in humans from in vivo preclinical and in vitro data to optimize drug candidates and dose regimens for further development. The prediction of oral pharmacokinetic behavior prior to initiation of clinical studies would substantially reduce the time and research investment involved in the design of first-in-human clinical studies and would ultimately contribute to the development of safer drugs. This prediction is based on the incorporation of drug permeability and metabolism data and enterocytic blood flow together with zonal and cellular heterogeneous distribution of metabolic enzymes and efflux/uptake transporters in the intestine and liver.

Education & Post-Doctoral Training

2005-2006

Postdoctoral Research Associate
School of Pharmacy
University of Washington, Seattle

2004-2005

Postdoctoral Research Associate
College of Pharmacy
University of Michigan, Ann Arbor

2004

Ph.D.

Clinical Pharmacy/Translational Research School of Pharmaceutical Sciences
Nagasaki University, Japan

2001

M.S.
Pharmaceutical Sciences School of Pharmaceutical Sciences
Nagasaki University, Japan

Academic Appointments

2007 - 2013	Assistant Professor, Department of Basic Pharmaceutical Sciences College of Pharmacy, University of Louisiana Monroe.
2013 - 06/2017	Associate Professor, Department of Basic Pharmaceutical Sciences College of Pharmacy, University of Louisiana Monroe.
07/2017	Professor, Department of Basic Pharmaceutical Sciences School of Pharmacy, University of Louisiana Monroe.
08/2017 - 11/2024	Professor, Department of Drug Discovery and Development Harrison College of Pharmacy, Auburn University.
12/2024 - present	Professor, Department of Pharmacology and Toxicology Medical College of Georgia, Augusta University.

Scientific Appointments

2024-present NIH/NIA reviewer. Study section AN-W (55) - Neurovascular, Metabolic, and Related Factors in the
Pathophysiology of AD/ADRD.

2024 NIH/NIA Review Panel on Research and Entrepreneurial Development Immersion (SBIR/STTR; March 2024),
Ad hoc.

2024- Guest Editor, Special issue in Molecular Immunology section, Neuroinflammation in the Pathogenesis of
Alzheimer's Disease and Related Dementias, second edition. International Journal of Molecular Sciences

2023-2024 Guest editor, Special issue in section Bioactives and Nutraceuticals, Olive Oil and Derivatives for Human Health.
International Journal of Molecular Sciences.

2022-2023 Guest Editor, Special issue on Research topic Model-Informed Drug Development and Evidence-Based
Translational Pharmacology. Frontiers in Pharmacology.

2021-2023 Guest Editor, Special issue in Molecular Immunology section, Neuroinflammation in the Pathogenesis of
Alzheimer's Disease and Related Dementias. International Journal of Molecular Sciences.

2021-2023 National Science Foundation reviewer, Phase I: Therapeutic Molecules.

2021 Guest Editor, Model-Informed Drug Development and Evidence-Based Translational Pharmacology, Frontiers in
Pharmacology - section Translational Pharmacology.

2020-2021 National Science Foundation reviewer, Phase I: COVID 19 - Drug Discovery, Delivery, and Manufacturing.

2020-2021 Guest Editor, Special issue in Molecular Neurobiology section, The Blood-Brain Barrier in Health and Disease.
International Journal of Molecular Sciences.

2016-2017 Guest Editor, Special issue in Molecular Pathology, Diagnostics, and Therapeutics section, Amyloid-beta and
Neurological Diseases, International Journal of Molecular Sciences.

2007-present Alzheimer’s Association, Reviewer.

Honors

Olive Wellness Institute Olive Science Research Award (2022)
Faculty Research Excellence Award, Auburn University (2018, 2024)
Bronze award for best researcher in health/medical research on EVOO, oleocanthal, and other phenols presented by the Oleocanthal International Society. Olympia, Greece; June 2-4 (2016).
Junior Scientist Program Award from the American and Malaysian Palm Oil Councils (2011).
Travel award from AAPS for “AAPS workshop on drug transporters in ADME: from the bench to the bedside”. Parsippany, New Jersey, USA (2005).
Outstanding graduate student research award of Nagasaki University, Japan (2004).
The Ministry of Education, Culture, Sports, Science and Technology of Japanese Government Scholarship, Japan (1998-2004).

Selected Publications

Book chapters

Ayoub NM, Khalil RW, Kaddoumi A (corresponding author). “α-Tocopherol for Alzheimer’s disease” in Nutrition and Neurological Disorders. Editor: Martin C, Patel VB, Preedy VR. Elsevier Publications, 2023. ISBN: 9780443186240

Al Rihani S., Batarseh Y, Yang E, Kaddoumi A (corresponding author). “Oleocanthal and neurological effects” in Olive Oil in Health and Disease Prevention, 2nd Edition. Editors: Watson RS, Preedy VR. Elsevier publications. 2021. ISBN: 978-0-12-819528-4.

Abuznait A, Qosa H, Mohamed LA, Batarseh YS, Kaddoumi A (corresponding author). “Neuroprotective effects of olive oil components in Alzheimer disease” in Neuroprotective Effects of Phytochemicals in Neurological disorders. Editors: Farooqui T, Farooqui AA. Wiley Blackwell. 2017.

Selected Publications

Alkhalifa AE, Al-Ghraiybah NF, Kaddoumi A. Extra-Virgin Olive Oil in Alzheimer's Disease: A Comprehensive Review of Cellular, Animal, and Clinical Studies. Int J Mol Sci. 2024;25(3):1914. doi: 10.3390/ijms25031914. PMID: 38339193; PMCID: PMC10856527.

Alkhalifa AE, Al-Ghraiybah NF, Odum J, Shunnarah JG, Austin N, Kaddoumi A. Blood-Brain Barrier Breakdown in Alzheimer's Disease: Mechanisms and Targeted Strategies. Int J Mol Sci. 2023; 24(22):16288. doi: 10.3390/ijms242216288. PMID: 38003477; PMCID: PMC10671257.

Abdallah IM, Al-Shami KM, Alkhalifa AE, Al-Ghraiybah NF, Guillaume C, Kaddoumi A. Comparison of Oleocanthal-Low EVOO and Oleocanthal against Amyloid-β and Related Pathology in a Mouse Model of Alzheimer's Disease. Molecules. 2023; 28(3):1249. doi: 10.3390/molecules28031249.PMID: 3677092.

Zhao J, Zhu X, Tan S, Chen C, Kaddoumi A, Guo XL, Lin YW, Cheung SYA. Editorial: Model-informed drug development and evidence-based translational pharmacology. Front Pharmacol. 2022; 13:1086551.

Kaddoumi A, Denney TS Jr, Deshpande G, Robinson JL, Beyers RJ, Redden DT, Praticò D, Kyriakides TC, Lu B, Kirby AN, Beck DT, Merner ND. Extra-Virgin Olive Oil Enhances the Blood-Brain Barrier Function in Mild Cognitive Impairment: A Randomized Controlled Trial. Nutrients. 2022; 14(23):5102.

Al-Ghraiybah NF, Wang J, Alkhalifa AE, Roberts AB, Raj R, Yang E, Kaddoumi A. Glial Cell-Mediated Neuroinflammation in Alzheimer's Disease. Int J Mol Sci. 2022; 23(18):10572. doi: 10.3390/ijms231810572.

Abdallah IM, Al-Shami KM, Yang E, Wang J, Guillaume C, Kaddoumi A. Oleuropein-Rich Olive Leaf Extract Attenuates Neuroinflammation in the Alzheimer's Disease Mouse Model. ACS Chem Neurosci. 2022;13(7):1002-1013.

Darakjian LI,* Rigakou A,* Brannen A, Qusa MH, Tasiakou N, Diamantakos P, Reed MN, Panizzi P, Boersma MD, Melliou E, El Sayed KA, Magiatis P, Kaddoumi A. Spontaneous In Vitro and In Vivo Interaction of (−)-Oleocanthal with Glycine in Biological Fluids: Novel Pharmacokinetic Markers. ACS Pharmacology & Translational Science 2021; 4, 179-192.

Wani A,* Al Rihani SB,* Sharma A, Weadick B, Govindarajan R, Khan SU, Sharma PR, Dogra A, Nandi U, Reddy CN, Bharate SS, Singh G, Bharate SB, Vishwakarma RA, Kaddoumi A, Kumar A. Crocetin promotes clearance of amyloid-β by inducing autophagy via the STK11/LKB1-mediated AMPK pathway. Autophagy. 2021; 19:1-20. doi: 10.1080/15548627.2021.1872187.

Mousa YM, Abdallah IM, Hwang M, Martin DR, Kaddoumi A. Amylin and pramlintide modulate γ-secretase level and APP processing in lipid rafts. Scientific Reports. 2020; 10(1):3751. doi: 10.1038/s41598-020-60664-5.

Al Rihani SB, Lan RS, Kaddoumi A. Granisetron Alleviates Alzheimer’s Disease Pathology in TgSwDI Mice Through Calmodulin-Dependent Protein Kinase II/cAMP-Response Element Binding Protein Pathway. J Alzheimer’s Disease. 2019; 72(4):1097-1117.

Al Rihani SB, Darakjian LI, Kaddoumi A. Oleocanthal-Rich Extra-Virgin Olive Oil Restores the Blood-Brain Barrier Function through NLRP3 Inflammasome Inhibition Simultaneously with Autophagy Induction in TgSwDI Mice. ACS Chemical Neuroscience. 2019; 10(8):3543-3554.

Nair S, Strohecker AM, Persaud AK, Bissa B, Muruganandan S, McElroy C, Pathak R, Williams M, Raj R, Kaddoumi A, Sparreboom A, Beedle AM, Govindarajan R. Adult stem cell deficits drive Slc29a3 disorders in mice. Nature Communication. 2019; 10(1):2943.

Elfakhri KH, Abdallah MI, Brannen AD, Kaddoumi A. Multi-faceted therapeutic strategy for treatment of Alzheimer's disease by concurrent administration of etodolac and α-tocopherol. Neurobiology of Disease. 2019; 125:123-134.

Wani A, Gupta M, Ahmad M, Shah AM, Ahsan AU, Qazi PH, Malik F, Singh GH, Sharma PR, Kaddoumi A, Bharate SB, Vishwakarma RA, Kumar A. Alborixin clears amyloid-β by inducing autophagy through PTEN mediated inhibition of AKT pathway. Autophagy. 2019. doi: 10.1080/15548627.2019.1596476.

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Amal Kaddoumi, PhD

Members of the Lab

Research Interest

Education & Post-Doctoral Training

2005-2006

2004-2005

2004

2001

Academic Appointments

Scientific Appointments

Honors

Selected Publications

Complete list of publications

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