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慢分裂肿瘤干细胞可能是造成某些癌症复发的元凶

已有 4301 次阅读 2012-6-2 01:57 |个人分类:科技视窗|系统分类:论文交流| 肿瘤, 以色列, cancer, patients

      为什么一些癌症患者在经过化疗获得缓解后肿瘤依然就会复发?这个问题长期以来一直让肿瘤学家们争论不休。本周发表在《血液》杂志的一项研究,发现在某些特定的血液肿瘤,慢分裂肿瘤干细胞可以摆脱通常针对快分裂细胞的化学治疗的影响,是以后癌症复发的根源。
 
论文摘要
Blood. 2012 May 29. [Epub ahead of print]
Cell lineage analysis of acute leukemia relapse uncovers the role of replication-rate heterogeneity and miscrosatellite instability.
Abstract

Human cancers display substantial intra-tumoral genetic heterogeneity, which facilitates tumor survival under changing microenvironmental conditions. Tumor substructure and its impact on disease progression and relapse are incompletely understood. In the current study, a high-throughput method that utilizes neutral somatic mutations accumulated in individual cells to reconstruct cell lineage trees was applied to hundreds of cells of human acute leukemia harvested from multiple patients at diagnosis and at relapse. The reconstructed cell lineage trees of acute myeloid leukemia (AML) patients demonstrated that leukemia cells at relapse were shallow (divide rarely) compared to cells at diagnosis and were closely related to their stem cell subpopulation, implying that in these instances relapse might have originated from rarely-dividing stem cells. In contrast, among acute lymphoid leukemia (ALL) patients, no differences in cell depth were observed between diagnosis and relapse. In one case of chronic myeloid leukemia (CML), at blast crisis, most of the cells at relapse were mismatch-repair deficient. In almost all leukemia cases, more than one lineage was observed at relapse, indicating that diverse mechanisms can promote relapse in the same patient. In conclusion, diverse relapse mechanisms can be observed by systematic reconstruction of cell lineage trees of leukemia patients.

 
 
请看科学家杂志对此项研究的评论
 
Why Some Cancers Come Back

 

By Cristina Luiggi | May 31, 2012

 

Why cancer comes back in some patients after chemotherapy has beaten it into remission has been a matter of debate for oncologists. In a new study published in Blood this week, researchers at The Weizmann Institute of Science in Rehovot, Israel, found that in certain blood cancers, slowly-dividing cancer stem cells that are impervious to the actions of chemotherapy—which commonly target fast-dividing cells—are the source for future recurring cancers.

Led by computational biologist Ehud Shapiro, the researchers reconstructed lineage trees of cells sampled from patients with newly diagnosed leukemia and from patients in which leukemia had returned. They found that in some cases, the source of the recurring cancer cells were not rapidly dividing cancer cells that had dodged chemotherapy, but the slowly-dividing stem cells at the root of the tree.

“We know that in many cases, chemotherapy alone is not able to cure leukemia,” Shapiro said in a press release. “Our results suggest that to completely eliminate it, we must look for a treatment that will not only eliminate the rapidly dividing cells, but also target the cancer stem cells that are resistant to conventional treatment.”

 



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