Clinical implications of cytosine deletion of exon 5 of P53 gene in non small cell lung cancer patients

Author:

Mir Rashid1,Masroor Mirza2,Javid Jamsheed1,Ahamad Imtiyaz2,Farooq Shazia2,Yadav Prasant2,Zuberi Mariyam2,Lone Maqbool3,Ray P.C2,Saxena Alpana2

Affiliation:

1. Prince Fahd Bin Sultan Research Chair Cancer Molecular Genetics, Department of Medical Laboratory Technology, Faculty of Applied Medical Sciences University of Tabuk

2. Cancer Genetic Lab, Department of Biochemistry, Maulana Azad Medical College and Associated Hospitals, New Delhi

3. Department of Radiation oncology, SKIMS, Jammu and Kashmir

Abstract

Abstract Aim: Lung cancer is considered to be the most common cancer in the world. In humans, about 50% or more cancers have a mutated tumor suppressor p53 gene thereby resulting in accumulation of p53 protein and losing its function to activate the target genes that regulate the cell cycle and apoptosis. Extensive research conducted in murine cancer models with activated p53, loss of p53, or p53 missense mutations have facilitated researchers to understand the role of this key protein. Our study was aimed to evaluate the frequency of cytosine deletion in nonsmall cell lung cancer (NSCLC) patients. Methods: One hundred NSCLC patients were genotyped for P53 (exon5, codon168) cytosine deletion leading to loss of its function and activate the target genes by allele-specific polymerase chain reaction. The P53 cytosine deletion was correlated with all the clinicopathological parameters of the patients. Results and Analysis: 59% cases were carrying P53 cytosine deletion. Similarly, the significantly higher incidence of cytosine deletion was reported in current smokers (75%) in comparison to exsmoker and nonsmoker. Significantly higher frequency of cytosine deletion was reported in adenocarcinoma (68.08%) than squamous cell carcinoma (52.83%). Also, a significant difference was reported between p53 cytosine deletion and metastasis (64.28%). Further, the majority of the cases assessed for response carrying P53 cytosine deletion were found to show faster disease progression. Conclusion: The data suggests that there is a significant association of the P53 exon 5 deletion of cytosine in codon 168 with metastasis and staging of the disease.

Publisher

Georg Thieme Verlag KG

Subject

Cancer Research,Oncology

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