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Titanium dioxide nanoparticles provide protection against polycyclic aromatic hydrocarbon BaP and chrysene‐induced perturbation of DNA repair machinery: A computational biology approach
Author(s) -
Dhasmana Anupam,
Jamal Qazi Mohd. Sajid,
Gupta Richa,
Siddiqui Mohd. Haris,
Kesari Kavindra Kumar,
Wadhwa Gulshan,
khan Saif,
Haque Shafiul,
Lohani Mohtashim
Publication year - 2015
Publication title -
biotechnology and applied biochemistry
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.468
H-Index - 70
eISSN - 1470-8744
pISSN - 0885-4513
DOI - 10.1002/bab.1388
Subject(s) - chrysene , aryl hydrocarbon receptor , pyrene , chemistry , benzo(a)pyrene , carcinogen , dna damage , dna repair , polycyclic aromatic hydrocarbon , dna , biochemistry , stereochemistry , environmental chemistry , organic chemistry , transcription factor , gene
We examined the interaction of polycyclic hydrocarbons (PAHs) like benzo‐α‐pyrene (BaP), chrysene, and their metabolites 7,8‐dihydro‐7,8‐dihydroxybenzo(a)pyrene,9,10‐oxide (BPDE) and chrysene 1,2‐diol‐3,4‐epoxide‐2 (CDE), with the enzymes involved in DNA repair. We investigated interaction of 120 enzymes with PAHs and screened out 40 probable targets among DNA repair enzymes, on the basis of higher binding energy than positive control. Out of which, 20 enzymes lose their function in the presence of BaP, chrysene, and their metabolites, which may fetter DNA repair pathways resulting in damage accumulation and finally leading to cancer formation. We propose the use of nanoparticles as a guardian against the PAH's induced toxicity. PAHs enter the cell via aryl hydrocarbon receptor (AHR). TiO 2 NP showed a much higher docking score with AHR (12,074) as compared with BaP and chrysene with AHR (4,600 and 4,186, respectively), indicating a preferential binding of TiO 2 NP with the AHR. Further, docking of BaP and chrysene with the TiO 2 NP bound AHR complex revealed their strong adsorption on TiO 2 NP itself, and not on their original binding site (at AHR). TiO 2 NPs thereby prevent the entry of PAHs into the cell via AHR and hence protect cells against the deleterious effects induced by PAHs.

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