Comparative Study of ERK1/2, Bcl2, and Sorcin with Clinicopathological Characteristics of Gastric carcinoma: Tubular Adenocarcinoma Vs Signet Ring Cell Carcinoma.
Sushmita Ghosh, Jayanta Chakrabarti, Partha Nath, Raya Banerjee, Neyaz Alam, Vilas D Nasare
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引用次数: 0
Abstract
Background and objective: Altered expression of tissue-specific tumor markers is associated with clinicopathological factors and poor clinical outcomes in Gastric Cancer (GC). However, the markers have been scarcely explored in the context of the distinct GC subtypes, which are crucial for assessing treatment response. This study explores the nuanced differences between gastric tubular adenocarcinoma (TA) and signet ring cell carcinoma (SRCC), focusing on the correlation of ERK1/2, Bcl2, and Sorcin expression. The aim is to identify potential differences between the subtypes and assess the prognostic value of the markers in relation to clinicopathological outcomes.
Methods: Immunohistochemistry evaluated the ERK1/2, Bcl2 and Sorcin expression in 78 patients (TA=37, SRCC=33; other=8) diagnosed with advanced non-metastatic GC. Descriptive statistics and correlations were assessed between the proteins and clinicopathological features. Overall survival and hazard risk (HR) were determined using Kaplan-Meier and Cox proportional hazard analyses.
Results: Higher ERK1/2 (66%) and lower Bcl2 (51%) expression was demonstrated in SRCC, whereas the opposite trend was noted in TA cases. On the contrary, Sorcin expression was high in both, however, predominant in SRCC (66%). Notably, post-NACT, the expression of these proteins was elevated. Significant difference in survival between TA (22±3.03 months) and SRCC (12±1.62 months) (p=0.007) was observed. In SRCC, higher ERK1/2, Sorcin, and low Bcl2 expressions were associated with shorter survival with HR>1 (p<0.05). Significant correlation between Sorcin and clinicopathological factors was analysed both in TA and SRCC (p<0.001) compared to ERK1/2 and Bcl2 expression. Sorcin expression was further associate with treatment response in non-responders (post-NACT) in both TA and SRCC (p<0.05).
Conclusion: High ERK1/2, Sorcin, and low Bcl2 expression prevailed in SRCC cases. These expressions were upregulated post-NACT in both subtypes. SRCC patients had shorter OS, moreover expression of ERK1/2, Sorcin, and Bcl2 correlated with poor survival outcomes and major clinicopathological factors in SRCC cases.
期刊介绍:
Cancer is a very complex disease. While many aspects of carcinoge-nesis and oncogenesis are known, cancer control and prevention at the community level is however still in its infancy. Much more work needs to be done and many more steps need to be taken before effective strategies are developed. The multidisciplinary approaches and efforts to understand and control cancer in an effective and efficient manner, require highly trained scientists in all branches of the cancer sciences, from cellular and molecular aspects to patient care and palliation.
The Asia Pacific Organization for Cancer Prevention (APOCP) and its official publication, the Asia Pacific Journal of Cancer Prevention (APJCP), have served the community of cancer scientists very well and intends to continue to serve in this capacity to the best of its abilities. One of the objectives of the APOCP is to provide all relevant and current scientific information on the whole spectrum of cancer sciences. They aim to do this by providing a forum for communication and propagation of original and innovative research findings that have relevance to understanding the etiology, progression, treatment, and survival of patients, through their journal. The APJCP with its distinguished, diverse, and Asia-wide team of editors, reviewers, and readers, ensure the highest standards of research communication within the cancer sciences community across Asia as well as globally.
The APJCP publishes original research results under the following categories:
-Epidemiology, detection and screening.
-Cellular research and bio-markers.
-Identification of bio-targets and agents with novel mechanisms of action.
-Optimal clinical use of existing anti-cancer agents, including combination therapies.
-Radiation and surgery.
-Palliative care.
-Patient adherence, quality of life, satisfaction.
-Health economic evaluations.
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