TY  - BOOK
AU  - Mona Mahmoud Ali Bekheet, 
AU  - Ismail Abdelshafy Abdelhamid
AU  - Mohamed Attia Ragheb
AU  -  Marwa Hasan Soliman
TI  - Synthesis, Molecular Docking, and Biological Activity Study of Some Unsaturated Carbonyl Derivatives Containing N and/or S Elements / 
U1  - 572 
PY  - 2023///
KW  - Biochemistry
KW  - qmark
KW  - Cyanoacrylamide
KW  -  Antiproliferative activity
KW  - Apoptosis
KW  - Cell cycle arrest
KW  - Docking
KW  -  DNA binding
N1  - Thesis (M.Sc.) Cairo University, 2023.; Bibliography: pages 95-118.; Issued also as CD
N2  - Five novel cyanoacrylamides incorporating sulphamethoxazole (5-9) were synthesized and characterized by various spectral analysis tools. The antiproliferative properties of the synthesized derivatives towards three human cancer cell lines (HCT116, MDA-MB-231 and A549) have been evaluated using MTT viability assay. Compound 9, incorporating 4-(piperidin-1-yl)phenyl moiety, showed the highest potency against the three cell lines compared to doxorubicin. Flow cytometric analysis revealed that compound 9 could effectively induce apoptosis and cell cycle arrest at the S phase in HCT116 cells. Compound 9 could also suppress the migration of HCT116 cells in wound healing assay. The mechanistic studies suggested that compound 9 exerted its anticancer activity through inducing HCT116 cells apoptosis by up-regulating Bax and caspase-3, down-regulating Bcl2 and survivin, blocking cell cycle in the S phase by downregulating cyclin A1, and inhibiting migration by upregulating CDH1. Using UV-Vis and EB-displacement measurements, compound 9 could interact with CT-DNA through a moderate intercalative mode. Moreover, the molecular docking confirmed that compound 9 had good binding affinities toward the active site of different proteins (Bcl2, CDK2 and CDH1). In summary, 9 is introduced as a promising antitumor lead candidate that is worthy of further drug efficacy improvement and preclinical studies.; ÙØ°Ø§ Ø§ÙØ¹ÙÙ ÙØªØ¶ÙÙ ØªØµÙÙØ¹ Ø³ÙØ³ÙØ©  Ø¬Ø¯ÙØ¯Ø© ÙÙ ÙØ±ÙØ¨Ø§Øª cyanoacrylamide Ø§ÙÙØ±ØªØ¨Ø·Ø© Ø¨ sulphamethoxazole Ø¹Ø¨Ø± ØªÙØ§Ø¹Ù Knoevenagel condensation Ø§ÙØ°Ù ÙØªØ¶ÙÙ ØªÙØ§Ø¹Ù  aldehydes Ù sulphamethoxazole ÙÙ Ø­ÙØ¶ Ø§ÙØ£Ø³ÙØªÙÙ ÙÙ ÙØ¬ÙØ¯ Ø£Ø³ÙØªØ§Øª Ø§ÙØµÙØ¯ÙÙÙ. ÙÙ ÙØ°Ù Ø§ÙØ¯Ø±Ø§Ø³Ø© Ø ØªÙ ØªØµÙÙØ¹ Ø³ÙØ³ÙØ© Ø¬Ø¯ÙØ¯Ø© ÙÙ cyanoacrylamide Ø§ÙÙØ±ØªØ¨Ø·Ø© Ø¨ÙØ´ØªÙØ§Øª sulphamethoxazole (5-9) ÙØªÙÙÙÙÙØ§ ÙØ¹ÙØ§ÙÙ ÙÙÙØ© ÙØ¶Ø§Ø¯Ø© ÙÙØ³Ø±Ø·Ø§Ù Ø¶Ø¯ ÙØ¬ÙÙØ¹Ø© ÙÙ Ø®Ø·ÙØ· Ø§ÙØ®ÙØ§ÙØ§ Ø§ÙØ³Ø±Ø·Ø§ÙÙØ© (MDA-MB-231 Ù A549 Ù HCT116).  ÙÙØ¯ ÙÙØ­Ø¸ Ø£Ù Ø§ÙÙØ±ÙØ¨ (9)Ø§ÙÙØ­ØªÙÙ Ø¹ÙÙ 4-(piperidin-1-yl)phenyl moiety Ø§ÙØ«Ø±ÙÙ ÙØ´Ø§Ø·Ø§Ù Ø¶Ø¯ Ø§ÙØ®ÙØ§ÙØ§ Ø§ÙØ³Ø±Ø·Ø§ÙÙØ© Ø ÙÙØ¹ ØªÙØ§Ø«Ø± Ø®Ø· Ø§ÙØ®ÙØ§ÙØ§ HCT116 Ø¨ÙØ§Ø¹ÙÙØ© Ø£ÙØ¶Ù ÙÙØ§Ø±ÙØ© Ø¨Ø§ doxorubicin. ÙØ¬Ø¯ Ø£Ù (9) ÙØ³Ø¨Ø¨ ÙÙØª Ø§ÙØ®ÙØ§ÙØ§ ÙØªÙÙÙ Ø¯ÙØ±Ø© Ø§ÙØ®ÙÙØ© ÙÙ Ø§ÙÙØ±Ø­ÙØ© S ÙÙ Ø®ÙØ§ÙØ§ HCT116. Ø£ÙØ¶ÙØ§ Ø ÙØ§Ù Ø§ÙÙØ±ÙØ¨ (9) Ø¨ØªÙÙÙÙ  cell migration Ø¨Ø´ÙÙ ÙØ¨ÙØ±. Ø¹ÙØ§ÙØ© Ø¹ÙÙ Ø°ÙÙ Ø ÙØ§Ù Ø§ÙÙØ±ÙØ¨ (9) Ø¨Ø²ÙØ§Ø¯Ø© ØªØµÙÙØ¹ Ø§ÙØ¨Ø±ÙØªÙÙØ§Øª Ø§ÙÙØ­ÙØ²Ø© ÙØ¹ÙÙÙÙ apoptosis  ÙØ«Ù Bax Ù CDH1 Ù caspase-3 Ø Ø¨ÙÙÙØ§ ØªÙ ØªÙÙÙÙ ØªØµÙÙØ¹  Bcl2 Ù survivin Ù cyclin A1 Ø¨Ø´ÙÙ ÙØ¨ÙØ±. Ø£ÙØ¶ÙØ§ Ø Ø£Ø¸ÙØ±Øª Ø¬ÙÙØ¹ Ø§ÙÙØ±ÙØ¨Ø§Øª Ø ÙÙØ§ Ø³ÙÙØ§ (5) Ù (9) Ø photocleavage activity Ø¶Ø¯ DNA pBR322 Ø§ÙØ¨ÙØ§Ø²ÙÙØ¯. ÙÙØ¸ÙØ± Ø§ÙÙØ±ÙØ¨ (9) ÙØ¯Ø±Ø© intercalating with CT-DNA Ø¨Ø§Ø³ØªØ®Ø¯Ø§Ù 	UV-Vis Ù EB quenching measurements. Ø  Ù ÙÙ Ø®ÙØ§Ù Ø§ÙØ¯Ø±Ø§Ø³Ù Ø§ÙÙØ¸Ø±ÙÙ Docking Studies Ø§Ø«Ø¨ØªØª Ø§Ù Ø§ÙÙØ±ÙØ¨ (9) ÙÙ ÙØ¯Ø±Ø© Ø¹Ø§ÙÙÙ Ø¹ÙÙ Ø§ÙØ¥Ø±ØªØ¨Ø§Ø· Ø¨Ø¨Ø¹Ø¶ Ø§ÙØ¨Ø±ÙØªÙÙØ§Øª ÙØ«Ù Bcl2  Ù  Cdk2Ù CDH1  ÙØªØ´ÙØ± ÙØ°Ù Ø§ÙØ¯Ø±Ø§Ø³Ø© Ø¥ÙÙ Ø£Ù Ø§ÙÙØ±ÙØ¨ (9) ÙØ¯ ÙÙÙÙ ÙÙ Ø§ÙÙØ¯Ø±Ø© Ø¹ÙÙ Ø§ÙØ¹ÙÙ ÙØ¯ÙØ§Ø¡ ÙØ¹ÙØ§Ø¬ Ø³Ø±Ø·Ø§Ù Ø§ÙÙÙÙÙÙ
ER  -