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一种用于乳腺癌的糖疗法的诞生。

BIRTH OF A GLYCOTHERAPY FOR BREAST CANCER.

作者信息

Banerjee Dipak K

机构信息

Department of Biochemistry, School of Medicine, University of Puerto Rico, Medical Sciences Campus, San Juan, PR 00936-5067, USA.

出版信息

Trends Carbohydr Res. 2023;15:25-37.

Abstract

Breast cancer is the most common malignant disease in women and is worldwide. The incidence rate of women's breast cancer in 2020 was 2,261,419 and 2022 estimates diagnosing 1,918,030 cases. The disease is heterogeneous and the pathogenesis of breast cancer still remains unclear. Much progress has been made in early detection and better treatment to improve survival. Unfortunately, the current treatment strategies destroy the patient's quality of life. The patients develop drug resistance, exhibit severe side effects, and not afford the cost creates anxiety among the patients, families, and friends. In addition, a considerable number of patients relapse as a result of organ metastasis, e.g., the triple-negative breast cancer (TNBC, ER/PRHER2). The 5-year survival rate of patients who recurred with distant metastasis is less than 20%. More than half a million women worldwide still suffer from metastatic breast cancer annually, and 90% of their deaths could be attributed to metastasis. One of the reasons for the failure of cancer therapeutics is the approaches did not consider the cancer holistically. All breast cancer cells and their micro environmental capillary endothelial cells express asparagine-linked (-linked) glycoproteins. We have tested a biologic and a small molecule, Tunicamycin-P (P = pure N-glycosylation inhibitor) to interfere with the protein -glycosylation pathway in the endoplasmic reticulum (ER) by specifically blocking the catalytic activity of -acetylglusosaminyl 1-phosphate transferase (GPT) activity. The outcome has been quantitative inhibition of and angiogenesis and the breast tumor progression of multiple subtypes in pre-clinical mouse models with "zero" toxicity. We have, therefore, concluded that Tunicamycin-P is expected to supersede the current therapeutics and become a Glycotherapy treating breast cancer of all subtypes.

摘要

乳腺癌是女性中最常见的恶性疾病,在全球范围内皆是如此。2020年女性乳腺癌的发病率为2261419例,2022年估计诊断出1918030例。该疾病具有异质性,乳腺癌的发病机制仍不清楚。在早期检测和更好的治疗以提高生存率方面已经取得了很大进展。不幸的是,目前的治疗策略破坏了患者的生活质量。患者会产生耐药性,出现严重的副作用,且费用负担不起,这给患者、家人和朋友带来了焦虑。此外,相当数量的患者会因器官转移而复发,例如三阴性乳腺癌(TNBC,雌激素受体/孕激素受体/人表皮生长因子受体2阴性)。远处转移复发患者的5年生存率低于20%。全球每年仍有超过50万女性患有转移性乳腺癌,其中90%的死亡可归因于转移。癌症治疗失败的原因之一是治疗方法没有从整体上考虑癌症。所有乳腺癌细胞及其微环境中的毛细血管内皮细胞都表达天冬酰胺连接(N-连接)的糖蛋白。我们测试了一种生物制剂和一种小分子衣霉素-P(P = 纯N-糖基化抑制剂),通过特异性阻断N-乙酰葡糖胺-1-磷酸转移酶(GPT)的催化活性来干扰内质网(ER)中的蛋白质糖基化途径。结果是在临床前小鼠模型中对多种亚型的肿瘤生长和血管生成进行了定量抑制,且具有“零”毒性。因此,我们得出结论,衣霉素-P有望取代目前的治疗方法,成为治疗所有亚型乳腺癌的糖疗法。

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