Zulfiqar Ahmad
A T Still University, USA
Keynote: J AIDS Clin Res
Introduction & Aim: Antibiotic resistance is posing an existential threat, as it will result in 10 million additional deaths
worldwide per year by 2050. Currently, about 700,000 people die every year from microbial infections. Thus, microbial
superbugs will become the top global killer, surpassing cancer. The impact of this public health crisis on the global economy
is projected to cost $ 100 trillion. The World Health Organizationâ??s global report on surveillance of antimicrobial resistance
estimated the yearly cost to the US health system to reach $ 34 billion. Fast-encroaching antibiotic resistance by microbes
in general and E. coli in particular is the main reason for this situation. Thus, finding alternative ways to kill microbes is
of paramount importance. Selective inhibition of microbial ATP synthase provides an effective and efficient way to combat
antibiotic resistant microbial infections. ATP synthase is the fundamental source of cellular energy production for almost all
organisms. Inhibition of ATP synthase can deprive cells of required energy leading to cell death. A wide variety of inhibitors
including phytochemicals and peptides are known to bind and inhibit ATP synthase. These phytochemicals and peptides bind
to the specific binding pockets on ATP synthase. These binding pockets are flanked by many variable amino acids in different
organisms. Our lab is identifying and characterizing phytochemicals and peptides as potent and selective inhibitors of ATP
synthase to combat the antibiotic resistant microbial infections using E. coli as a model organism.
Method: Wild type, null and mutant E. coli growth properties are being tested on fermentable glucose and non-fermentable
succinate carbon sources. Wild type and mutant enzymes were isolated by harvesting cells in the minimal media. Inhibitory
studies are performed on membrane bound F1Fo ATP synthase. Structural modifications of inhibitors are made through
replacement or re-positioning of the functional groups (â??OH, â??COOH, â??NH2, â??NO2, â??PO4) on phytochemicals or addition
of positive charges on the peptides. Wild type and mutant cell growth assays are tested in presence and absence of inhibitors
along with null control.
Results: We found that phytochemicals and peptides cause variable degree of inhibition of ATP synthase. Modification of
inhibitors augments extent of inhibition. In phytochemicals, re-positioning and addition of new functional groups and for
peptides, addition of a c-terminal NH2 group enhances the inhibitory potency. We also observed that incremental addition of
positively charged residues in peptides augments the inhibitory effects of peptides by about 100-fold. Growth of E. coli strains
in presence and absence inhibitors suggest that ATP synthase is a potent molecular drug target to combat microbial infections.
It is also explored the synergistic inhibitory effects of phytochemicals and peptides on microbial ATP synthase.
Conclusion: It is concluded that ATP synthase is a potent molecular drug target and selective inhibition of microbial ATP
synthase by phytochemicals and peptides can be used to combat drug resistant microbial infections.
Zulfiqar Ahmad has obtained his Doctorate in Biosciences from Jamia Millia Islamia, New Delhi and became Faculty at Hamdard University, New Delhi. In 1998, he has joined as a Postdoctoral Fellow at the University of Rochester Medical Center, NY. In 2006, he was appointed Faculty Position at East Tennessee State University. In 2010, he moved to Alabama A&M University and in 2013 joined A. T. Still University. His research focus is on the role of ATP synthase in human health and diseases, using Escherichia coli as a model system. The overall goal of his research is to demonstrate ATP synthase as a viable molecular target against drug resistant bacterial infections.
E-mail: Zahmad@atsu.edu
Journal of AIDS & Clinical Research received 5061 citations as per Google Scholar report
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