Department of Medicine, Division of Hematology and Oncology, Tisch Cancer Institute at Mount Sinai, New York, New York, USA.
Clin Cancer Res. 2011 Sep 15;17(18):5850-7. doi: 10.1158/1078-0432.CCR-10-2574. Epub 2011 Jun 14.
Systemic minimal residual disease after primary tumor treatment can remain asymptomatic for decades. This is thought to be due to the presence of dormant disseminated tumor cells (DTC) or micrometastases in different organs. DTCs lodged in brain, lungs, livers, and/or bone are a major clinical problem because they are the founders of metastasis, which ultimately kill cancer patients. The problem is further aggravated by our lack of understanding of DTC biology. In consequence, there are almost no rational therapies to prevent dormant DTCs from surviving and expanding. Several cancers, including melanoma as well as breast, prostate, and colorectal carcinomas, undergo dormant periods before metastatic recurrences develop. Here we review our experience in studying the cross-talk between ERK1/2 and p38α/β signaling in models of early cancer progression, dissemination, and DTC dormancy. We also provide some potential translational and clinical applications of these findings and describe how some currently used therapies might be useful to control dormant disease. Finally, we draw caution on the use of p38 inhibitors currently in clinical trials for different diseases as these may accelerate metastasis development.
原发肿瘤治疗后,全身性微小残留病灶可能在数十年内无症状。这被认为是由于休眠的播散性肿瘤细胞(DTC)或不同器官中的微转移存在。DTC 定居在脑、肺、肝和/或骨中是一个主要的临床问题,因为它们是转移的创始者,最终导致癌症患者死亡。我们对 DTC 生物学缺乏了解,使问题进一步恶化。因此,几乎没有合理的治疗方法来防止休眠的 DTC 存活和扩张。一些癌症,包括黑色素瘤以及乳腺癌、前列腺癌和结直肠癌,在转移复发发展之前经历休眠期。在这里,我们回顾了我们在研究 ERK1/2 和 p38α/β 信号在早期癌症进展、扩散和 DTC 休眠模型中的相互作用方面的经验。我们还提供了这些发现的一些潜在的转化和临床应用,并描述了目前用于控制休眠性疾病的一些治疗方法可能如何有用。最后,我们提请注意目前在不同疾病临床试验中使用的 p38 抑制剂,因为这些抑制剂可能会加速转移的发展。
