Title : design synthesis and biological evaluation of some substituted pyrazole derivatives as anti tubercular agents

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Type of Material:	Thesis
Title:	design synthesis and biological evaluation of some substituted pyrazole derivatives as anti tubercular agents
Researcher:	Mitali Hardik Jasani
Guide:	Patel, L. J.
Department:	FACULTY OF PHARMACY
Publisher:	Ganpat University
Place:	Mehsana
Year:	2023
Language:	English
Subject:	Clinical Medicine
	Pharmacy
	Clinical Pre Clinical and Health
	Critical Care Medicine
	Pharmacy
	Medical and Health Sciences
Dissertation/Thesis Note:	PhD; FACULTY OF PHARMACY, Ganpat University, Mehsana; 2023; 18276011006
Fulltext:	Shodhganga

000 00000ctm a2200000ua 4500
001 455333
003 IN-AhILN
005 2024-09-26 16:56:50
008 __ 240924t2023||||ii#||||g|m||||||||||eng||
035 __ |a(IN-AhILN)th_455333
040 __ |aGANU_384012|dIN-AhILN
041 __ |aeng
100 __ |aMitali Hardik Jasani|eResearcher
110 __ |aFACULTY OF PHARMACY|bGanpat University|dMehsana|ein|0U-0132
245 __ |adesign synthesis and biological evaluation of some substituted pyrazole derivatives as anti tubercular agents
260 __ |aMehsana|bGanpat University|c2023
300 __ |a20624 KB|dDVD
500 __ |aMycobacterium tuberculosis, Pyrazole, CYP121A1, Molecular docking, MmpL3
502 __ |o18276011006|bPhD|cFACULTY OF PHARMACY, Ganpat University, Mehsana|d2023
518 __ |oDate of Award|d2024
518 __ |oDate of Registration|d2018
518 __ |oDate of Viva-voce|d2023-12-28
518 __ |oDate of Notification|d2023-12-28
520 __ |aDiscovering new drugs with novel targets is vital for the success of treatment of tuberculosis as antibiotic resistance is increasing among the TB population. Mycobacterium tuberculosis cytochrome P450 CYP121A1 is a promising drug target for the treatment of tuberculosis owing to its essential role in mycobacterium growth. Using a rational approach, that includes molecular docking studies of some substituted pyrazole derivatives a series of pyrazole analogue were designed and pass through computational studies. Compound with good docking score and ADME profile were synthesized using two step reaction and biologically evaluated for their inhibitory activity towards M. tuberculosis. All compounds were analyzed by IR, LCMS, 1H-NMR and 13C- NMR. Among them 5 compounds shows significant activity having MIC (3.12 to 6.25µg/ml). Synthesized compound were re-docked with MmpL3 protein to identify dual inhibitory approach. All synthesized compounds gives good docking score and shows dual inhibition acts on cellular
650 __ |aPharmacy|2UGC
650 __ |aMedical and Health Sciences|2AIU
653 __ |aClinical Medicine
653 __ |aPharmacy
653 __ |aClinical Pre Clinical and Health
653 __ |aCritical Care Medicine
700 __ |aPatel, L. J.|eGuide
856 __ |uhttp://shodhganga.inflibnet.ac.in/handle/10603/563570|yShodhganga
905 __ |afromsg

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000	00000ctm a2200000ua 4500
001	455333
003	IN-AhILN
005	2024-09-26 16:56:50
008	__	240924t2023\|\|\|\|ii#\|\|\|\|g\|m\|\|\|\|\|\|\|\|\|\|eng\|\|
035	__	\|a(IN-AhILN)th_455333
040	__	\|aGANU_384012\|dIN-AhILN
041	__	\|aeng
100	__	\|aMitali Hardik Jasani\|eResearcher
110	__	\|aFACULTY OF PHARMACY\|bGanpat University\|dMehsana\|ein\|0U-0132
245	__	\|adesign synthesis and biological evaluation of some substituted pyrazole derivatives as anti tubercular agents
260	__	\|aMehsana\|bGanpat University\|c2023
300	__	\|a20624 KB\|dDVD
500	__	\|aMycobacterium tuberculosis, Pyrazole, CYP121A1, Molecular docking, MmpL3
502	__	\|o18276011006\|bPhD\|cFACULTY OF PHARMACY, Ganpat University, Mehsana\|d2023
518	__	\|oDate of Award\|d2024
518	__	\|oDate of Registration\|d2018
518	__	\|oDate of Viva-voce\|d2023-12-28
518	__	\|oDate of Notification\|d2023-12-28
520	__	\|aDiscovering new drugs with novel targets is vital for the success of treatment of tuberculosis as antibiotic resistance is increasing among the TB population. Mycobacterium tuberculosis cytochrome P450 CYP121A1 is a promising drug target for the treatment of tuberculosis owing to its essential role in mycobacterium growth. Using a rational approach, that includes molecular docking studies of some substituted pyrazole derivatives a series of pyrazole analogue were designed and pass through computational studies. Compound with good docking score and ADME profile were synthesized using two step reaction and biologically evaluated for their inhibitory activity towards M. tuberculosis. All compounds were analyzed by IR, LCMS, 1H-NMR and 13C- NMR. Among them 5 compounds shows significant activity having MIC (3.12 to 6.25µg/ml). Synthesized compound were re-docked with MmpL3 protein to identify dual inhibitory approach. All synthesized compounds gives good docking score and shows dual inhibition acts on cellular
650	__	\|aPharmacy\|2UGC
650	__	\|aMedical and Health Sciences\|2AIU
653	__	\|aClinical Medicine
653	__	\|aPharmacy
653	__	\|aClinical Pre Clinical and Health
653	__	\|aCritical Care Medicine
700	__	\|aPatel, L. J.\|eGuide
856	__	\|uhttp://shodhganga.inflibnet.ac.in/handle/10603/563570\|yShodhganga
905	__	\|afromsg