en Cancer Biology Cancer Biology مقاله کامل Full Length/Original Article <div style="text-align: justify;"><span style="font-family:Times New Roman;"><span style="font-size:11pt"><span style="line-height:normal"><b><span style="font-size:10.5pt">Background:</span></b><span style="font-size:10.5pt"> INPP5A is involved in&nbsp;different cellular events, including cell proliferation. Since <i>INPP5A</i>, <i>HLAG1</i>, <i>IL-10</i>, and <i>MMP-21</i> genes play fundamental roles in ESCC tumorigenesis, we aimed in this study to clarify the possible interplay of these genes and explore the potential of these chemistries as a predictor marker for diagnosis in ESCC disease. </span></span></span><br> <span style="font-size:11pt"><span style="line-height:normal"><b><span style="font-size:10.5pt">Methods: </span></b><span style="font-size:10.5pt">Gene expression analysis of <i>INPP5A</i>, <i>HLAG</i>-<i>1</i>, <i>IL-10</i>, and <i>MMP-21</i> was performed using relative comparative real-time PCR in 56 ESCCs compared to their margin normal tissues. Immunohistochemical staining was accomplished for INPP5A in ESCCs. Analysis of ROC curves and the AUC were applied to evaluate the diagnostic capability of the candidate genes. </span></span></span><br> <span style="font-size:11pt"><span style="line-height:normal"><b><span style="font-size:10.5pt">Results:</span></b><span style="font-size:10.5pt"> High levels of <i>HLA-G1</i>, <i>MMP-21</i>, and <i>IL-10</i> were detected in nearly 23.2%, 62.5%, and 53.5% of ESCCs compared to the normal tissues, respectively, whereas <i>INPP5A</i> underexpression was detected in 19.6% of ESCCs, which all tested genes indicated significant correlations with each other. The protein expression level of INPP5A in ESCC tissues was significantly lower than that of the non-tumor esophageal tissues (<i>p</i> = 0.001). Interestingly, the concomitant expression of the <i>INPP5A/HLA-G1, INPP5A</i>/<i>MMP-21, INPP5A</i>/<i>IL-10, HLA-G1</i>/<i>MMP-21, HLA-G1</i>/<i>IL-10</i>, and <i>MMP</i>-21/IL-10 was significantly correlated with several clinicopathological variables. <i>INPP5A</i>, <i>HLA-G1</i>, <i>MMP-21</i>, and <i>IL-10</i> showed to be the most appropriate candidates to discriminate tumor/non-tumor groups due to the total AUCs of all combinations (>60%). </span></span></span><br> <b><span style="font-size:10.5pt"><span style="line-height:107%">Conclusion:</span></span></b><span style="font-size:10.5pt"><span style="line-height:107%"> Our results represent a new regulatory axis containing <i>INPP5A/HLAG-1/IL-10/MMP-21</i> markers in ESCC development and may provide novel insight into the mechanism of immune evasion mediated by the <i>INPP5A/HLAG-1/IL-10/MMP-21</i> regulatory network in the disease.</span></span></span></div> 440 453 http://ibj.pasteur.ac.ir/browse.php?a_code=A-10-4696-66&slc_lang=en&sid=1 Sima Ardalan Khales Yes Immunology Research Center, Mashhad University of Medical Sciences, Mashhad, Iran Azadeh Aarabi No Immunology Research Center, Mashhad University of Medical Sciences, Mashhad, Iran Mohammad Reza Abbaszadegan No Medical Genetics Research Center, Mashhad University of Medical Sciences, Mashhad, Iran; Mohammad Mahdi Forghanifard No Department of Biology, Damghan Branch, Islamic Azad University, Damghan, Iran