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Visualizing the dynamic of adoptively transferred T cells during the rejection of large established tumors.

机译:可视化动态传输的收养T细胞在建立大型的拒绝肿瘤。

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摘要

Adoptive T-cell therapy (ATCT) can result in tumor rejection, yet the behavior and fate of the introduced T cells remain unclear. We developed a novel bioluminescence mouse model, which enabled highly sensitive detection of T-cell signals at the single-cell level. Transferred T cells preferentially accumulated within antigen-positive tumors, relative to the unaffected areas in each mouse, and remarkably, expanded within both lymphopenic and P14 mice. This expansion was controlled and efficient, as evaluated by bioluminescence imaging (BLI) of the T-cell signals and by tumor rejection respectively. Analysis of the population dynamics of transferred T cells in ATCT of large tumors revealed that proliferation did not always follow a simple linear pattern of expansion, but showed an oscillating pattern of expansion and contraction that was often followed by a rebound, until full tumor rejection was achieved. Furthermore, visualizing the recall response showed that the transferred T cells responded expeditiously, indicating the ability of these cells to survive, establish memory and compete with endogenous T cells for as long as 1 year after rejecting the tumor.
机译:收养t细胞疗法(ATCT)会导致肿瘤拒绝,然而的行为和命运介绍了T细胞仍不明朗。新颖的生物荧光小鼠模型,使高度敏感的t细胞信号检测单细胞水平。优先积累在相对于抗原阳性肿瘤每个鼠标未受影响的地区,值得注意的是,扩大在lymphopenic和好老鼠。这种扩张和有效的控制,评估生物荧光成像(BLI)和肿瘤抑制t细胞信号分别。正规的大型肿瘤的T细胞转移表明扩散并不总是遵循一个简单的线性扩张的模式,但显示一个振荡的扩张和模式收缩通常是紧随其后的是一个反弹,直到全部肿瘤排斥。此外,可视化召回响应表明,T细胞的反应迅速,说明这些的能力细胞生存,建立内存和竞争与内生T细胞只要1年遭拒绝后,肿瘤。

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