首页> 外文期刊>Molecular cancer therapeutics >Tumor-associated CD75s- and iso-CD75s-gangliosides are potential targets for adjuvant therapy in pancreatic cancer.
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Tumor-associated CD75s- and iso-CD75s-gangliosides are potential targets for adjuvant therapy in pancreatic cancer.

机译:肿瘤相关的CD75s和异CD75s神经节苷脂是胰腺癌辅助治疗的潜在靶标。

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Pancreatic adenocarcinoma confers one of the highest mortality rates in malignant human tumors with very poor prognosis. Because as yet no treatments are available that produce a substantial survival benefit for this fatal neoplasia, new therapeutic concepts are urgently required to support cancer standard treatment. In search of tumor-associated gangliosides with therapeutic background, we probed a random collection of cancerous and adjacent normal postoperative tissue samples from 38 patients for the expression of CD75s- and iso-CD75s-gangliosides. We exhaustively analyzed the expression of CD75s-1-ganglioside (IV(6)Neu5Ac-nLc4Cer) and structurally closely related iso-CD75s-1-ganglioside (IV(3)Neu5Ac-nLc4Cer) by means of immunohistology of cryosections and semiquantitative TLC of tissue lipid extracts combined with mass spectrometry. CD75s-1- and iso-CD75s-1-ganglioside showed an elevated expression in 42% and 66% of the tumors, respectively, indicating a significant association with neoplastic transformation (P = 0.001). Thus, increased expression of CD75s-1- and iso-CD75s-1-gangliosides renders these cell surface molecules promising candidates for oncologic applications. Further statistical analysis revealed a significant enhancement of CD75s-1-ganglioside in the group of less differentiated tumors (grade >2) suggesting this ganglioside as a potential marker for poor differentiation. The CD75s-specific antitumor drug rViscumin, which represents the recombinant counterpart of the ribosome-inactivating lectin viscumin, has successfully passed clinical phase I trials and provides an opportunity for treating pancreatic cancer. Consequently, if an enhanced expression is existent in malignant tissues, we propose the targeting of CD75s-gangliosides with rViscumin as a novel potential strategy in adjuvant treatment of pancreatic malignancies.
机译:胰腺腺癌是预后非常差的恶性人类肿瘤中最高的死亡率之一。由于尚无可用于治疗这种致命性瘤形成的实质性生存获益的治疗方法,因此迫切需要新的治疗方案来支持癌症标准治疗。为寻找具有治疗背景的肿瘤相关神经节苷脂,我们从38位患者中随机收集了癌性和邻近正常术后组织样本的CD75s和iso-CD75s神经节苷脂的表达。我们通过冷冻切片的免疫组织学方法和半定量TLC分析了CD75s-1-神经节苷脂(IV(6)Neu5Ac-nLc4Cer)和与结构紧密相关的iso-CD75s-1-神经节苷脂(IV(3)Neu5Ac-nLc4Cer)的表达。组织脂质提取物与质谱联用。 CD75s-1-和iso-CD75s-1-神经节苷脂分别在42%和66%的肿瘤中表达升高,表明与肿瘤转化显着相关(P = 0.001)。因此,CD75s-1-和异CD75s-1-神经节苷脂的表达增加使得这些细胞表面分子有望成为肿瘤学应用的候选物。进一步的统计分析表明,在分化程度较低的肿瘤组(> 2级)中,CD75s-1-神经节苷脂显着增强,表明该神经节苷脂是分化不良的潜在标志。 CD75s特异性抗肿瘤药物rViscumin代表了核糖体失活的凝集素viscumin的重组对应物,已成功通过I期临床试验,并为治疗胰腺癌提供了机会。因此,如果在恶性组织中存在增强的表达,我们建议用rViscumin靶向CD75s-神经节苷脂作为胰腺癌辅助治疗中的一种新的潜在策略。

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