Department of Basic Medical Science, College of Medicine, Prince Sattam Bin Abdulaziz University, Al-Kharj, Postal Code:11942, Saudi Arabia.
Department of Clinical Laboratory Sciences, College of Applied Medical Sciences, King Saud University, Riyadh, Saudi Arabia.
Cell Mol Biol (Noisy-le-grand). 2020 Dec 31;66(8):26-32.
There are very scanty reports on gastro-intestinal stromal tumors (GISTs), a very common tumor of mesenchymal cells in GIT track primary resistance to imatinib. This comprehensive study identifies the prevalence, clinical presentation and GIST genotype association in the imatinib naïve population. Prospectively a record of anthropometric, baseline demographic data and clinical details for the patients diagnosed with GIST were scrutinized. Pathological information included the presence or absence of necrosis, tumor size, mitotic counts, immune-histochemical staining for CD 34, CD 117 and DOG1 was performed using biopsy sample. Selected exon genes of KIT, PDGFRA and BRAF were amplified and subjected to mutation analysis by direct sequencing. Appropriate statistical analyses were performed. The male/female ratio was 1.8:1 among 54 patients with GIST. The mean GIST size was comparatively bigger in females (2.49±0.855) than males (2.26±1.13). The stomach was the most common site for GIST followed by the Small bowel and rectum. The majority of the tumours were spindle cell. This study reports 12 different types of mutation among 39 KIT, 8 PDGFRA and 7 BRAF mutations. In KIT, the most prevalent was exon 11 mutation with the KITdelinc557/558 (14/30) being the major exon 11 type mutation. In PDGRFA, five exons 18 with p.D842V substitution and three exons 12 deletion mutation was reported. Seven patients had strong or diffuse BRAF staining having V600E type mutation as major BRAF type mutation. Drug-resistant GIST due to acquired mutations remains a serious issue, therefore genetic information of such mutational related to drug-resistant may provide the imperative clue for diagnosis and clinical treatment. These mutations are pivotal for prognosis and associated with imatinib as not all of them but only a few are reported resistant to the imatinib.
胃肠道间质瘤(GISTs)是一种非常常见的胃肠道间质细胞肿瘤,对伊马替尼具有原发性耐药。本研究全面分析了初治伊马替尼患者中 GIST 的流行率、临床表现和 GIST 基因型相关性。前瞻性地记录了诊断为 GIST 的患者的人体测量、基线人口统计学数据和临床详细信息。病理信息包括有无坏死、肿瘤大小、有丝分裂计数、CD34、CD117 和 DOG1 的免疫组织化学染色,均使用活检样本进行检测。对 KIT、PDGFRA 和 BRAF 的选定外显子基因进行扩增,并通过直接测序进行突变分析。进行了适当的统计分析。54 例 GIST 患者中,男女比例为 1.8:1。女性 GIST 平均大小(2.49±0.855)大于男性(2.26±1.13)。胃是 GIST 最常见的部位,其次是小肠和直肠。大多数肿瘤为梭形细胞。本研究报告了 39 例 KIT、8 例 PDGFRA 和 7 例 BRAF 突变中的 12 种不同类型的突变。在 KIT 中,最常见的是外显子 11 突变,其中 KITdelinc557/558(14/30)是主要的外显子 11 类型突变。在 PDGRFA 中,报告了 5 个外显子 18 与 p.D842V 取代和 3 个外显子 12 缺失突变。7 例患者存在 BRAF 强烈或弥漫性染色,主要 BRAF 类型突变是 V600E 型突变。获得性突变导致的耐药性 GIST 仍然是一个严重的问题,因此与耐药性相关的遗传信息可能为诊断和临床治疗提供必要的线索。这些突变对于预后至关重要,并与伊马替尼相关,因为并非所有突变都对伊马替尼耐药,只有少数突变报告耐药。
