Your search keyword '"Milik, Sandra N."' showing total 3 results

1. SAR investigation and optimization of benzimidazole-based derivatives as antimicrobial agents against Gram-negative bacteria.

Author

Dokla, Eman M.E., Abutaleb, Nader S., Milik, Sandra N., Kandil, Ezzat A.E.A., Qassem, Omar M., Elgammal, Yehia, Nasr, Maha, McPhillie, Martin J., Abouzid, Khaled A.M., Seleem, Mohamed N., Imming, Peter, and Adel, Mai

Subjects

*BENZIMIDAZOLES, *GRAM-negative bacteria, *ANTIBACTERIAL agents, *ANTI-infective agents, *COLISTIN, *GRAM-negative bacterial diseases, *ESCHERICHIA coli, *DRUG resistance in bacteria

Abstract

Antibiotic-resistant bacteria represent a serious threat to modern medicine and human life. Only a minority of antibacterial agents are active against Gram-negative bacteria. Hence, the development of novel antimicrobial agents will always be a vital need. In an effort to discover new therapeutics against Gram-negative bacteria, we previously reported a structure-activity-relationship (SAR) study on 1,2-disubstituted benzimidazole derivatives. Compound III showed a potent activity against tolC -mutant Escherichia coli with an MIC value of 2 μg/mL, representing a promising lead for further optimization. Building upon this study, herein, 49 novel benzimidazole compounds were synthesized to investigate their antibacterial activity against Gram-negative bacteria. Our design focused on three main goals, to address the low permeability of our compounds and improve their cellular accumulation, to expand the SAR study to the unexplored ring C, and to optimize the lead compound (III) by modification of the methanesulfonamide moiety. Compounds (25a-d , 25f-h , 25k , 25l , 25p , 25r , 25s , and 26b) exhibited potent activity against tolC -mutant E. coli with MIC values ranging from 0.125 to 4 μg/mL, with compound 25d displaying the highest potency among the tested compounds with an MIC value of 0.125 μg/mL. As its predecessor, III , compound 25d exhibited an excellent safety profile without any significant cytotoxicity to mammalian cells. Time-kill kinetics assay indicated that 25d exhibited a bacteriostatic activity and significantly reduced E. coli JW55031 burden as compared to DMSO. Additionally, combination of 25d with colistin partially restored its antibacterial activity against Gram-negative bacterial strains (MIC values ranging from 4 to 16 μg/mL against E. coli BW25113, K. pneumoniae , A. baumannii , and P. aeruginosa). Furthermore, formulation of III and 25d as lipidic nanoparticles (nanocapsules) resulted in moderate enhancement of their antibacterial activity against Gram-negative bacterial strains (A. Baumannii, N. gonorrhoeae) and compound 25d demonstrated superior activity to the lead compound III. These findings establish compound 25d as a promising candidate for treatment of Gram-negative bacterial infections and emphasize the potential of nano-formulations in overcoming poor cellular accumulation in Gram-negative bacteria where further optimization and investigation are warranted to improve the potency and broaden the spectrum of our compounds. [Display omitted] • An extensive SAR study was established for the lead compound III. • Compound 25d showed potent activity against tolC-mutant E. coli. • 25d is a bacteriostatic agent with excellent safety profile. • Combination of 25d with colistin manifested synergistic activity against Gram-negative bacteria. • 25d nanocapsule formulation improved its activity against some Gram-negative wild strains. [ABSTRACT FROM AUTHOR]

Published

2023

2. Discovery of a benzimidazole-based dual FLT3/TrKA inhibitor targeting acute myeloid leukemia.

Author

Dokla, Eman M.E., Abdel-Aziz, Amal Kamal, Milik, Sandra N., McPhillie, Martin J., Minucci, Saverio, and Abouzid, Khaled A.M.

Subjects

*ACUTE myeloid leukemia, *CELL death, *WESTERN immunoblotting, *PROTEIN-tyrosine kinases, *SMALL molecules, *CELL cycle

Abstract

[Display omitted] • A benzimidazole derivative with nanomolar activity against FLT3 and TrKA kinase. • 4ACP was identified via scaffold hopping & structural simplification of quizartinib. • 4ACP prompted apoptotic and necrotic cell death and G0/G1 cell cycle arrest. • 4ACP exhibited selective antiproliferative profile and low toxicity in normal cells. • 4ACP represents a novel FLT3/TrKA dual kinase inhibitor for targeted therapy of AML. FMS-like tyrosine kinase 3 (FLT3) enzyme overexpression and mutations are the most common molecular abnormalities associated with acute myeloid leukemia (AML). In addition, recent studies investigated the role of tropomyosin receptor kinase A (TrKA) enzyme fusions in promoting AML growth and survival. Based on these premises, targeting both kinases using dual inhibitors would constitute a promising therapeutic approach to target resistant AML. Guided by ligand-based design and structure simplification of the FLT3 inhibitor, quizartinib, we developed a benzimidazole-based small molecule, 4ACP , that exhibited nanomolar activity against wild-type FLT3, FLT3-Internal tandem duplications (FLT3-ITD), and FLT3-D835Y (FLT3-TKD) mutation (IC 50 = 43.8, 97.2, and 92.5 nM respectively). Additionally, 4ACP demonstrated potent activity against colon cancer KM12 cell line (IC 50 = 358 nM) and subsequent mechanistic deconvolution identified TrKA enzyme as a second plausible target (IC 50 = 23.6 nM) for our compound. 4ACP manifested preferential antiproliferative activity against FLT3-ITD positive AML cell lines (MV4-11 IC 50 = 38.8 ± 10.7 nM and MOLM-13 IC 50 = 54.9 ± 4.1 nM), while lacking activity against FLT3-ITD negative AML cell lines. Western blot analysis confirmed 4ACP ability to downregulate ERK1/2 and mTOR signaling downstream of FLT3-ITD in AML cells. Furthermore, 4ACP prompted apoptotic and necrotic cell death and G0/G1 cell cycle arrest as indicated by cell cycle analysis. 4ACP did not show cytotoxic effects on normal BNL and H9c2 cells and demonstrated decreased activity against c-Kit enzyme, hence, indicating lower probability of synthetic lethal toxicity and a relatively safer profile. In light of these data, 4ACP represents a novel FLT3/TrKA dual kinase inhibitor for targeted therapy of AML. [ABSTRACT FROM AUTHOR]

Published

2022

3. Development of benzimidazole-based derivatives as antimicrobial agents and their synergistic effect with colistin against gram-negative bacteria.

Author

Dokla, Eman M.E., Abutaleb, Nader S., Milik, Sandra N., Li, Daoyi, El-Baz, Karim, Shalaby, Menna-Allah W., Al-Karaki, Rawan, Nasr, Maha, Klein, Christian D., Abouzid, Khaled A.M., and Seleem, Mohamed N.

Subjects

*GRAM-negative bacteria, *ANTI-infective agents, *BENZIMIDAZOLES, *COLISTIN, *ANTIBACTERIAL agents, *BENZIMIDAZOLE derivatives, *CELL lines

Abstract

Gram-negative bacteria pose a distinctive risk worldwide, especially with the evolution of major resistance to carbapenems, fluoroquinolones and colistin. Therefore, development of new antibacterial agents to target Gram-negative infections is of utmost importance. Using phenotypic screening, we synthesized and tested thirty-one benzimidazole derivatives against E. coli JW55031 (TolC mutant strain). Compound 6c showed potent activity with MIC value of 2 μg/ml, however, it lacked activity against several Gram-negative microbes with intact efflux systems, including E. coli BW25113 (wild-type strain). Combination of 6c with colistin partially restored its antibacterial activity against wild strains (MIC range, 8–16 μg/ml against E. coli , K. pneumoniae , A. baumannii , and P. aeruginosa). 6c exhibited no cytotoxicity against two mammalian cell lines. Therefore, compound 6c represents a promising lead for further optimization to overcome Gram-negative resistance alone or in combination therapy. Image 1 • Benzimidazole derivative, 6c is a promising lead to target Gram-negative bacteria. • Compound 6c shows potent activity against TolC mutant E. coli. • 6c and colistin manifest synergistic activity against Gram-negative bacteria. • Compound 6c shows no cytotoxicity on mammalian cell lines. [ABSTRACT FROM AUTHOR]

Published

2020