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上皮细胞内磷酸果糖激酶的重定位是乳腺癌复发前的一个新事件,能够准确预测患者的预后。

Relocation of phosphofructokinases within epithelial cells is a novel event preceding breast cancer recurrence that accurately predicts patient outcomes.

机构信息

Department of Ophthalmology and Visual Sciences, University of Michigan Medical School, Ann Arbor, Michigan.

出版信息

Am J Physiol Cell Physiol. 2021 Oct 1;321(4):C654-C670. doi: 10.1152/ajpcell.00176.2021. Epub 2021 Aug 4.

Abstract

Although recurrent cancers can become life threatening, little is known about the intracellular events required for cancer recurrences. Due to this lack of mechanistic information, there is no test to predict cancer recurrences or nonrecurrences during early stages of disease. In this retrospective study, we use ductal carcinoma in situ of the breast as a framework to better understand the mechanism of cancer recurrences using patient outcomes as the physiological observable. Conventional pathology slides were labeled with anti-phosphofructokinase type L (PFKL) and anti-phosphofructokinase/fructose-2,6-bisphosphatase type 4 (PFKFB4) reagents. PFKL and PFKFB4 were found in ductal epithelial cell nucleoli from DCIS samples of women who did not experience a cancer recurrence. In contrast, PFKL and PFKFB4 may be found near the plasma membrane in samples from patients who will develop recurrent cancer. With the use of machine learning to predict patient outcomes, holdout studies of individual patient micrographs for the three biomarkers PFKL, PFKFB4, and phosphorylated glucose transporter 1 (GLUT1) demonstrated 38.6% true negatives, 49.5% true positives, 11.9% false positives, and 0% false negatives ( = 101). A subpopulation of recurrent samples demonstrated PFKL, PFKFB4, and phosphorylated GLUT1 accumulation at the apical surface of epithelial cells, suggesting that carbohydrates can be harvested from the ducts' luminal spaces as an energy source. We suggest that PFK isotype patterns are metabolic switches representing key mechanistic steps of recurrences. Furthermore, PFK enzyme patterns within epithelial cells contribute to an accurate diagnostic test to classify DCIS patients as high or low recurrence risk.

摘要

虽然复发性癌症可能会危及生命,但人们对癌症复发所需的细胞内事件知之甚少。由于缺乏机制信息,目前还没有测试可以在疾病早期预测癌症的复发或非复发。在这项回顾性研究中,我们使用乳腺原位导管癌作为框架,通过将患者的预后作为生理可观察指标,更好地了解癌症复发的机制。常规病理切片用抗磷酸果糖激酶 L(PFKL)和抗磷酸果糖激酶/果糖-2,6-二磷酸酶 4(PFKFB4)试剂进行标记。在未经历癌症复发的女性 DCIS 样本的导管上皮细胞核仁中发现了 PFKL 和 PFKFB4。相比之下,在将发生复发性癌症的患者样本中,PFKL 和 PFKFB4 可能存在于靠近质膜的位置。通过使用机器学习来预测患者的预后,对三个生物标志物 PFKL、PFKFB4 和磷酸化葡萄糖转运蛋白 1(GLUT1)的单个患者显微照片进行留一法研究,结果显示 38.6%的真阴性、49.5%的真阳性、11.9%的假阳性和 0%的假阴性(=101)。复发性样本的一个亚群显示上皮细胞的顶表面有 PFKL、PFKFB4 和磷酸化 GLUT1 的积累,这表明可以从导管腔的腔隙中获取碳水化合物作为能量来源。我们认为,PFK 同工型模式是代谢开关,代表了复发的关键机制步骤。此外,上皮细胞内的 PFK 酶模式有助于进行准确的诊断测试,将 DCIS 患者分为高复发风险或低复发风险。

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