Broadening the scope of WEE1 inhibitors: identifying novel drug candidates via computational approaches and drug repurposing
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作者:
Chandrasekaran, Jaikanth
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Sri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, India
Sri Ramachandra Inst Higher Educ & Res Deemed be U, Dept Pharmacol, Chennai 600116, Tamil Nadu, IndiaSri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, India
Chandrasekaran, Jaikanth
[1
,4
]
Sivakumaresan, Yogeetha
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Sri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, IndiaSri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, India
Sivakumaresan, Yogeetha
[1
]
Shankar, Keerthika
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Sri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, IndiaSri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, India
Shankar, Keerthika
[1
]
Dickson, Melphiya
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Sri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, IndiaSri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, India
Dickson, Melphiya
[1
]
Kumar, Shruthi Laya Saravana
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Sri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, IndiaSri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, India
Kumar, Shruthi Laya Saravana
[1
]
Ramanathan, Lalitha
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Sri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, IndiaSri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, India
Ramanathan, Lalitha
[1
]
Ahmad, Iqrar
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机构:
Prof Ravindra Nikam Coll Pharm, Dept Pharmaceut Chem, Dhule, India
R C Patel Inst Pharmaceut Educ & Res, Dept Pharmaceut Chem, Div Comp Aided Drug Design, Shirpur, IndiaSri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, India
Ahmad, Iqrar
[2
,3
]
Patel, Harun
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R C Patel Inst Pharmaceut Educ & Res, Dept Pharmaceut Chem, Div Comp Aided Drug Design, Shirpur, IndiaSri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, India
Patel, Harun
[3
]
机构:
[1] Sri Ramachandra Inst Higher Educ & Res Deemed Be U, Dept Nephrol, Chennai, Tamil Nadu, India
WEE1;
kinase;
small molecule inhibitors;
e-pharmacophore model;
t-SNE distribution map;
analogue generation;
MD simulation;
TEMOZOLOMIDE;
D O I:
10.1080/07391102.2023.2251070
中图分类号:
Q5 [生物化学];
Q7 [分子生物学];
学科分类号:
071010 ;
081704 ;
摘要:
The protein kinase Wee1 plays a vital role in the G2/M cell cycle checkpoint activation, triggered by double-stranded DNA disruptions. It fulfills this task by phosphorylating and consequently deactivating the cyclin B linked to Cdk1/Cdc2 at the Tyr15 residue, leading to a G2 cell cycle halt and subsequent delay of mitosis post DNA damage. Despite advancements, only the Wee1 inhibitor MK1775 has made it to Phase II clinical trials, presenting a challenge in innovative chemical structure development for small molecule discovery. To navigate this challenge, we employed an e-pharmacophore model of the MK1775-WEE1 complex (PDB ID: 5V5Y), using in silico screening of FDA-approved drugs. We chose six drugs for analog creation, guided by docking scores, key residue interactions, and ligand occupancy. Utilizing the 'DrugSpaceX' database, we generated 2,776 analogues via expert-defined transformations. Our findings identified DE90612 as the top-ranked analogue, followed by DE363106, DE489678, DE395383, DE90548, DE689343, DE395019, and DE538066. These analogues introduced unique structures not found in other databases. A t-SNE structurally diversified distribution map unveiled promising transformations linked to Temozolomide for WEE1 inhibitor development. Simulations of the WEE1-DE90612 complex (a Temozolomide analogue) for 200 nanoseconds demonstrated stability, with DE90612 forging robust bonds with active site residues and sustaining vital contacts at ASN376 and CYS379. These results underscore DE90612's potential inhibitory properties at the WEE1 binding site, warranting additional in vitro and in vivo exploration for its anticancer activity. Our approach outlines a promising pathway for creating diverse WEE1 inhibitors with suitable biological properties for potential oncology therapeutics.Communicated by Ramaswamy H. Sarma
机构:
Univ Juarez Estado Durango, Fac Med & Nutr, Ave Univ & Fanny Anitua S-N, Durango 34000, MexicoUniv Juarez Estado Durango, Fac Med & Nutr, Ave Univ & Fanny Anitua S-N, Durango 34000, Mexico
Campos-Almazan, Mara Ibeth
Hernandez-Campos, Alicia
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机构:
Univ Nacl Autonoma Mexico, Fac Quim, Dept Farm, Ciudad De Mexico 04510, MexicoUniv Juarez Estado Durango, Fac Med & Nutr, Ave Univ & Fanny Anitua S-N, Durango 34000, Mexico
Hernandez-Campos, Alicia
Castillo, Rafael
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Univ Nacl Autonoma Mexico, Fac Quim, Dept Farm, Ciudad De Mexico 04510, MexicoUniv Juarez Estado Durango, Fac Med & Nutr, Ave Univ & Fanny Anitua S-N, Durango 34000, Mexico
Castillo, Rafael
Sierra-Campos, Erick
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Univ Juarez Estado Durango, Fac Ciencias Quim, Campus Gomez Palacio,Ave Articulo 123 S-N, Gomez Palacio 35010, MexicoUniv Juarez Estado Durango, Fac Med & Nutr, Ave Univ & Fanny Anitua S-N, Durango 34000, Mexico
Sierra-Campos, Erick
Valdez-Solana, Monica
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Univ Juarez Estado Durango, Fac Ciencias Quim, Campus Gomez Palacio,Ave Articulo 123 S-N, Gomez Palacio 35010, MexicoUniv Juarez Estado Durango, Fac Med & Nutr, Ave Univ & Fanny Anitua S-N, Durango 34000, Mexico
Valdez-Solana, Monica
Avitia-Dominguez, Claudia
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Univ Juarez Estado Durango, Fac Med & Nutr, Ave Univ & Fanny Anitua S-N, Durango 34000, MexicoUniv Juarez Estado Durango, Fac Med & Nutr, Ave Univ & Fanny Anitua S-N, Durango 34000, Mexico
Avitia-Dominguez, Claudia
Tellez-Valencia, Alfredo
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Univ Juarez Estado Durango, Fac Med & Nutr, Ave Univ & Fanny Anitua S-N, Durango 34000, MexicoUniv Juarez Estado Durango, Fac Med & Nutr, Ave Univ & Fanny Anitua S-N, Durango 34000, Mexico
机构:
Aligarh Muslim Univ, Fac Life Sci, Dept Biochem, Aligarh 202002, Uttar Pradesh, IndiaAligarh Muslim Univ, Fac Life Sci, Dept Biochem, Aligarh 202002, Uttar Pradesh, India
Zafar, Atif
Ahmad, Sabahuddin
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机构:
Jamia Millia Islamia, Fac Nat Sci, Dept Comp Sci, New Delhi 110025, IndiaAligarh Muslim Univ, Fac Life Sci, Dept Biochem, Aligarh 202002, Uttar Pradesh, India
Ahmad, Sabahuddin
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Rizvi, Asim
Ahmad, Masood
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Aligarh Muslim Univ, Fac Life Sci, Dept Biochem, Aligarh 202002, Uttar Pradesh, IndiaAligarh Muslim Univ, Fac Life Sci, Dept Biochem, Aligarh 202002, Uttar Pradesh, India
机构:
Sri Sankara Arts & Sci Coll, Res Dept Microbiol, Kanchipuram 631561, IndiaSri Sankara Arts & Sci Coll, Res Dept Microbiol, Kanchipuram 631561, India
Kavitha, Kuppuswamy
Sivakumar, Subramaniam
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Sri Sankara Arts & Sci Coll, Res Dept Biochem, Kanchipuram 631561, IndiaSri Sankara Arts & Sci Coll, Res Dept Microbiol, Kanchipuram 631561, India
Sivakumar, Subramaniam
Ramesh, Balasubramanian
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Sri Sankara Arts & Sci Coll, Res Dept Biotechnol, Kanchipuram 631561, IndiaSri Sankara Arts & Sci Coll, Res Dept Microbiol, Kanchipuram 631561, India
机构:
Taman Perindustrian UEP, Canc Res Initiat Fdn, Drug Discovery Lab, Subang Jaya 47600, Selangor Darul, MalaysiaJaypee Univ Informat Technol, Dept Pharm, Waknaghat 173234, India