Publications by authors named "Hina Aftab"

Article Synopsis
  • Dihydrofolate reductase (DHFR) is an important enzyme linked to folate metabolism, making it a key target for cancer and antimicrobial treatments.
  • Researchers synthesized a series of 4-pyrrolidine-based thiosemicarbazones and tested their ability to inhibit DHFR, finding that these compounds showed significant inhibitory effects with IC values ranging from 12.37 to 54.10 μM, with compound 5d being the most effective.
  • The study included molecular docking and ADME analysis to explore how these compounds bind to DHFR and to identify those with desirable properties for the development of new therapeutic agents.
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Dihydrofolate reductase (DHFR), an essential enzyme in folate metabolism, presents a promising target for drug development against various diseases, including cancer and tuberculosis. Herein, we present an integrated approach combining in vitro biochemical assays with in silico molecular docking analysis to evaluate the inhibitory potential of 4-piperidine-based thiosemicarbazones 5(a-s) against DHFR. In our in vitro study, a novel series of 4-piperidine-based thiosemicarbazones 5(a-s) were assessed for their inhibitory activity against DHFR enzyme.

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In the current study, three novel 1,4-phenylenediamine-based chromophores (3a-3c) were synthesized and characterized and then their nonlinear optical (NLO) characteristics were explored theoretically. The characterization was done by spectroscopic analysis, FT-IR, UV-Visible, and NMR spectroscopy, and elemental analysis. Notably, these chromophores exhibited UV-Visible absorption within the range of 378.

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