Design of PD-L1 inhibitors for lung cancer

Design of PD-L1 inhibitors for lung cancer

The progression of lung cancer is associated with inactivation of programmed cell death protein 1, abbreviated as PD- 1 which regulates the suppression of the body's immune system by suppressing T- cell inflammatory activity and is responsible for preventing cancer cell growth. It is of interes...

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Veröffentlicht in:Bioinformation 2019, Vol.15 (2), p.139-150
Hauptverfasser: Udhwani, Trishang, Mukherjee, Sourav, Sharma, Khushboo, Sweta, Jajoriya, Khandekar, Natasha, Nayarisseri, Anuraj, Singh, Sanjeev Kumar
Format: Artikel
Sprache:eng
Schlagworte:
Apoptosis
Cancer
Cell death
Cytotoxicity
Deactivation
Immune system
Inactivation
Inflammation
Inhibitors
Intestinal absorption
Intestine
Lung cancer
Molecular docking
Molecular structure
PD-1 protein
PD-L1 protein
Proteins
Toxicity
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Zusammenfassung:The progression of lung cancer is associated with inactivation of programmed cell death protein 1, abbreviated as PD- 1 which regulates the suppression of the body's immune system by suppressing T- cell inflammatory activity and is responsible for preventing cancer cell growth. It is of interest to identify inhibitors for PD-L1 dimeric structure through molecular docking and virtual screening. The virtual screened compound XGIQBUNWFCCMAS-UHFFFAOYSA-N (PubChem CID: 127263272) displays a high affinity with the target protein. ADMET analysis and cytotoxicity studies further add weight to this compound as a potential inhibitor of PD-L1. The established compound BMS-202 still shows the high re-rank score, but the virtual screened drug possesses a better ADMET profile with a higher intestinal absorption value and lower toxicity.
ISSN:0973-2063
0973-8894
0973-2063
DOI:10.6026/97320630015139