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Synthesis, molecular modeling and bio-evaluation of cycloalkyl fused 2-aminopyrimidines as antitubercular and antidiabetic agents
Authors:Singh Nimisha  Pandey Sarvesh Kumar  Anand Namrata  Dwivedi Richa  Singh Shyam  Sinha Sudhir Kumar  Chaturvedi Vinita  Jaiswal Natasa  Srivastava Arvind Kumar  Shah Priyanka  Siddiqui M Imran  Tripathi Rama Pati
Institution:a Medicinal and Process Chemistry Division, Central Drug Research Institute, CSIR, Lucknow 226 001, India
b Division of Drug Target Discovery and Development, Central Drug Research Institute, CSIR, Lucknow 226 001, India
c Biochemistry, Central Drug Research Institute, CSIR, Lucknow 226 001, India
d Molecular and Structure Biology Division, Central Drug Research Institute, CSIR, Lucknow 226 001, India
Abstract:An economical and efficient one step synthesis of a series of 8-(arylidene)-4-(aryl)-5,6,7,8-tetrahydro-quinazolin-2-ylamines and 9-(arylidene)-4-(aryl)-6,7,8,9-tetrahydro-5H-cycloheptapyrimidin-2-ylamines by the reaction of bis-benzylidene cycloalkanones and guanidine hydrochloride in presence of NaH has been developed. All the synthesized compounds were evaluated against Mycobacterium tuberculosis H37Rv strain and the α-glucosidase and glycogen phosphorylase enzymes. Few of the compounds have shown interesting in vitro activity with MIC up to 3.12 μg/mL against M. tuberculosis and very good inhibition of α-glucosidase and glycogen phosphorylase enzymes. The most potent non toxic compound 40 exhibited about 58% ex vivo activity at MIC of 3.12 μg/mL. The present study opens a new gate to synthesize antitubercular agents for diabetic TB patients. In silico docking studies indicate that mycobacterial dihydrofolate reductase is the possible target of these compounds.
Keywords:Cycloalkyl fused 2-aminopyrimidines  bis-Benzylidenecycloalkanones  α-Glucosidase inhibitor  Glycogen phosphorylase inhibitor  Antitubercular agents  DHFR inhibitor
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