The Validity of Immunohistochemistry in Detecting Microsatellite Instability in Pediatric Solid Neoplasms

Q3 Health Professions

Journal of Nature and Science of Medicine Pub Date : 2024-04-01 DOI:10.4103/jnsm.jnsm_61_23

Khaldoon Aljerian, Waleed AlRajban, Tariq Aljohani, Ali Alshehri, Omar Alsherif, Musa Alharbi, I. Abosoudah, W. Jastaniah, S. Daama, Abdulrahman AlSultan, Nahaa E. Alsubaie

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Abstract

The DNA mismatch repair (MMR) is the biological pathway that plays a key role in maintaining genomic stability during DNA replication and recombination. The value of MMR pathway is under investigation in pediatrics’ solid tumors. In this research work, we investigated the proteins involved in the oncogenesis of pediatric solid neoplasms and detect these proteins in a representative cohort sample of Saudi pediatric cases under the bioinformatic networking technique. We also described the MLH1, BRAF, p53, proliferating cell nuclear antigen, and PMS2 along with MSH2-MSH6 antibodies to be a diagnostic immunohistochemistry (IHC) panel for identifying MMR mutations. This research will open the new doors for advanced research on proteins involved in the oncogenesis of pediatric solid neoplasms. The hypotheses were tested on a sample of solid malignancies and IHC results were reported. The study was conducted in different institutions in Saudi Arabia. The inclusion criteria required enrolling biopsies of solid neoplasms or resected solid malignant neoplasms presented to the laboratories in the participating institutions of all pediatric patients (aging from 0 to 14 years). The specimens were examined microscopically utilizing Hematoxylin and Eosin stain as well as the utilization of MMR proteins immunohistochemistry (IHC), and PNCA. The qualitative assessment showed that IHC diagnosis yielded positive results with ≥80% of positive cells (intact) for MMR proteins (MSH2, MSH6, PMS2, and MLH1). The PCNA protein was absent only in vaginal germ cell tumor and metastatic medulloblastoma. In our sample, we have found that there is an intact MMR proteins expression. Also, the IHC technique presents accuracy and ability as a diagnostic technique for identifying the different types of pediatric cancers. The MMR protein panel accompanied with PCNA panels holds additional value, as it helps reduce dependency solely on MMR protein expressions.

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免疫组化在检测小儿实体瘤微卫星不稳定性中的有效性

DNA 错配修复（MMR）是一种生物途径，在 DNA 复制和重组过程中对维持基因组稳定性起着关键作用。MMR途径在儿科实体瘤中的价值正在研究之中。在这项研究工作中，我们调查了参与小儿实体瘤肿瘤发生的蛋白质，并利用生物信息网络技术在具有代表性的沙特小儿病例队列样本中检测了这些蛋白质。我们还描述了MLH1、BRAF、p53、增殖细胞核抗原、PMS2以及MSH2-MSH6抗体，这些抗体是鉴定MMR突变的免疫组化（IHC）诊断面板。这项研究将为儿科实体瘤致癌蛋白的高级研究打开一扇新的大门。研究人员对实体恶性肿瘤样本进行了假设检验，并报告了IHC结果。这项研究在沙特阿拉伯的不同机构进行。纳入标准要求将所有儿科患者（0-14 岁）的实体瘤或切除的实体恶性肿瘤活检样本提交给参与机构的实验室。标本在显微镜下使用苏木精和伊红染色法进行检查，并使用 MMR 蛋白免疫组织化学（IHC）和 PNCA 进行检测。定性评估显示，IHC 诊断结果呈阳性，MMR 蛋白（MSH2、MSH6、PMS2 和 MLH1）阳性细胞（完整）≥80%。只有阴道生殖细胞瘤和转移性髓母细胞瘤中没有 PCNA 蛋白。在我们的样本中，我们发现 MMR 蛋白表达完整。此外，IHC 技术作为一种诊断技术，在鉴别不同类型的儿科癌症方面具有准确性和能力。MMR 蛋白面板与 PCNA 面板的结合具有额外的价值，因为它有助于减少对 MMR 蛋白表达的单纯依赖。

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