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首页> 外文期刊>Molecular therapy: the journal of the American Society of Gene Therapy >A tubulin binding peptide targets glioma cells disrupting their microtubules, blocking migration, and inducing apoptosis
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A tubulin binding peptide targets glioma cells disrupting their microtubules, blocking migration, and inducing apoptosis

机译:微管蛋白结合肽靶向神经胶质瘤细胞,破坏其微管,阻断迁移并诱导凋亡

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摘要

Despite aggressive treatment regimes, glioma remains a largely fatal disease. Current treatment limitations are attributed to the precarious locations within the brain where such tumors grow, their highly infiltrative nature precluding complete resection and lack of specificity among agents capable of attenuating their growth. Here, we show that in vitro, glioma cells of diverse origins internalize a peptide encompassing a tubulin-binding site (TBS) on the neurofilament light protein. The internalized peptide disrupts the microtubule network, inhibits migration and proliferation, and leads to apoptosis. Using an intracerebral transplant model, we show that most, if not all, of these responses to peptide exposure also occur in vivo. Notably, a single intratumor injection significantly attenuates tumor growth, while neither peptide uptake nor downstream consequences are observed elsewhere in the host nervous system. Such preferential uptake suggests that the peptide may have potential as a primary or supplementary glioblastoma treatment modality by exploiting its autonomous microtubule-disrupting activity or engaging its capacity to selectively target glioma cells with other cell-disrupting cargos.
机译:尽管有积极的治疗方案,但神经胶质瘤仍然是致命的疾病。当前的治疗局限性归因于此类肿瘤生长的大脑内不稳定的位置,其高度浸润性,无法进行完全切除以及在能够减弱其生长的药物之间缺乏特异性。在这里,我们显示了体外,各种来源的神经胶质瘤细胞将包含神经丝轻蛋白上微管蛋白结合位点(TBS)的肽内化。内在化的肽破坏微管网络,抑制迁移和增殖,并导致凋亡。使用脑内移植模型,我们显示了大多数(即使不是全部)对肽暴露的反应也发生在体内。值得注意的是,单次肿瘤内注射显着减缓了肿瘤的生长,而在宿主神经系统的其他部位均未观察到肽摄取或下游后果。这样的优先摄取表明,通过利用其自主的破坏微管的活性或利用其选择性破坏胶质瘤细胞的能力与其他破坏细胞的肽结合,该肽可能具有作为原发性或补充性胶质母细胞瘤治疗方式的潜力。

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