Synthesis, molecular docking, antiplasmodial and antioxidant activities of new sulfonamido-pepetide derivatives
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作者:
Onoabedje, Efeturi A.
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Univ Nigeria, Fac Phys Sci, Dept Pure & Ind Chem, Nsukka, Enugu State, Nigeria
Cent Drug Res Inst, Div Med & Proc Chem, Lucknow, Uttar Pradesh, IndiaUniv Nigeria, Fac Phys Sci, Dept Pure & Ind Chem, Nsukka, Enugu State, Nigeria
Onoabedje, Efeturi A.
[1
,3
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Ibezim, Akachukwu
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Univ Nigeria, Fac Pharmaceut Sci, Dept Pharmaceut & Med Chem, Nsukka, Enugu State, NigeriaUniv Nigeria, Fac Phys Sci, Dept Pure & Ind Chem, Nsukka, Enugu State, Nigeria
Ibezim, Akachukwu
[2
]
Okoro, Uchechukwu C.
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Univ Nigeria, Fac Phys Sci, Dept Pure & Ind Chem, Nsukka, Enugu State, NigeriaUniv Nigeria, Fac Phys Sci, Dept Pure & Ind Chem, Nsukka, Enugu State, Nigeria
Okoro, Uchechukwu C.
[1
]
Batra, Sanjay
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Cent Drug Res Inst, Div Med & Proc Chem, Lucknow, Uttar Pradesh, IndiaUniv Nigeria, Fac Phys Sci, Dept Pure & Ind Chem, Nsukka, Enugu State, Nigeria
Batra, Sanjay
[3
]
机构:
[1] Univ Nigeria, Fac Phys Sci, Dept Pure & Ind Chem, Nsukka, Enugu State, Nigeria
[2] Univ Nigeria, Fac Pharmaceut Sci, Dept Pharmaceut & Med Chem, Nsukka, Enugu State, Nigeria
[3] Cent Drug Res Inst, Div Med & Proc Chem, Lucknow, Uttar Pradesh, India
Twenty-three new series of toluene-sulfonamide dipeptide derivatives were synthesized and screened for anti-plasmodial and antioxidant potencies. Many of the derivatives were active against Plasmodium falciparum with IC50 ranging from 3.20 - 9.10 mu M. The ability of compounds 7h, 7m and 7n (IC50 of 7.53, 7.21 and 6.01 mu g/mL respectively) to scavenge DPPH free radicals were comparable to that of ascorbic acid. Additionally, molecular docking disclosed that four compounds exhibited theoretical inhibition constant at submicromolar concentrations (K-i = 0.72, 0.75, 0.57, and 0.53 mu M respectively) compare to the reference ligand (a pyrazole sulfonamide; K-i = 0.01 mu M). Overall, some of the derivatives possess antimalarial property as well as the ability to inhibit oxidative stress in malaria pathophysiology; and hence, are good candidates for further antimalarial drug research.
机构:
Univ Johannesburg, Ctr Nat Prod Res CNPR, Dept Chem Sci, Doornfontein, ZA-2028 Johannesburg, South Africa
Univ Johannesburg, Dept Chem Sci, Drug Discovery & Smart Mol Res Lab, POB 17011, ZA-2028 Johannesburg, South AfricaUniv Johannesburg, Dept Chem Sci, POB 524 Pk, ZA-2006 Auckland Pk, South Africa
Ndinteh, Derek T.
Kolawole, Oyebamiji A.
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Bowen Univ, Dept Chem & Ind Chem, Iwo, Osun, NigeriaUniv Johannesburg, Dept Chem Sci, POB 524 Pk, ZA-2006 Auckland Pk, South Africa
Kolawole, Oyebamiji A.
Adeyinka, Adedapo S.
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Univ Johannesburg, Dept Chem Sci, POB 524 Pk, ZA-2006 Auckland Pk, South AfricaUniv Johannesburg, Dept Chem Sci, POB 524 Pk, ZA-2006 Auckland Pk, South Africa