Background: Metastatic cells from a primary tumor can occur before the primary cancer is detected. Metastatic cells can also remain in the patient for many years after removal of the primary tumor without proliferating. These dormant malignant cells can awaken and cause recurrent disease decades after the primary treatment. The purpose of this article is to review the clinical evidence for early dissemination and late recurrences in human malignant tumors. We used the following definitions: dormancy of cells may be defined as a nonproliferating state or an arrest in the cell cycle that results in a prolonged G0 phase. If one accepts the term “late metastases” to indicate a period exceeding 10 years from the removal of the primary tumor, then the two malignancies in which this occurs most frequently are cutaneous malignant melanoma (CMM) and renal cell carcinoma (RCC).Methods: PubMed, Web of Science, and Scopus were searched with the keywords “metastases,” “early dissemination,” “late recurrences,” “inadvertently transmitted cancer,” “tumor growth rate,” “dormancy,” “circulating tumor cells,” and “transplantation of cancer.”Results: Several case reports of early dissemination and late recurrences of various types of malignancies were found. Analyses of the growth rates of several malignant tumors in the original host indicated that the majority of cancers had metastasized years before they were detected. CMM, RCC, and malignant glioblastoma were the three most common malignancies resulting from an organ transplantation. CMM and RCC were also the two most common malignancies that showed dormancy. In several cases of transplanted CMM and RCC, the donor did not have any known malignancy or had had the malignancy removed so long ago that the donor was regarded as cured.Conclusion: (1) Metastases can frequently exist prior to the detection of the primary tumor. (2) Metastatic cells may reside in organs in the original host that are not usually the site of detectable secondary tumors, for example, the kidneys and heart. (3) Metastatic cells remain dormant for decades after the primary tumor has been removed. (4) Dormancy might be reversible and lead to late recurrences.
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机译:背景:原发肿瘤的转移细胞可以在检测到原发癌之前发生。转移性细胞在去除原发肿瘤后也可以在患者体内保留很多年而不会增殖。这些处于休眠状态的恶性细胞可在主要治疗后数十年醒来并引起疾病复发。本文的目的是回顾人类恶性肿瘤的早期传播和晚期复发的临床证据。我们使用以下定义:细胞的休眠可以定义为非增殖状态或导致G0期延长的细胞周期停滞。如果一个人接受术语“晚期转移”来表示原发肿瘤切除后超过10年,那么发生率最高的两个恶性肿瘤是皮肤恶性黑色素瘤(CMM)和肾细胞癌(RCC)。 :使用“转移”,“早期传播”,“晚期复发”,“无意间传播的癌症”,“肿瘤生长率”,“休眠”,“循环肿瘤细胞”等关键词搜索PubMed,Web of Science和Scopus。结果:发现了几例各种类型恶性肿瘤的早期传播和晚期复发的病例报告。对原始宿主中几种恶性肿瘤生长速率的分析表明,大多数癌症在被发现之前已经转移了几年。 CMM,RCC和恶性胶质母细胞瘤是器官移植导致的三种最常见的恶性肿瘤。 CMM和RCC也是表现出休眠的两个最常见的恶性肿瘤。在几例移植了CMM和RCC的病例中,供体没有任何已知的恶性肿瘤或很久以前就已去除了恶性肿瘤,因此该供体被认为已治愈。结论:(1)在发现原发灶之前,转移灶可能经常存在。瘤。 (2)转移细胞可能驻留在原始宿主的器官中,这些器官通常不是可检测到的继发性肿瘤的部位,例如肾脏和心脏。 (3)转移性细胞在原发肿瘤切除后仍保持休眠状态。 (4)休眠可能是可逆的,并导致晚期复发。
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