細(xì)胞治療使用的 lonza 04-418Q 無血清培養(yǎng)基 (點(diǎn)擊標(biāo)題進(jìn)入)
干細(xì)胞治療使用的 lonza 12-725F 無血清培養(yǎng)基 (點(diǎn)擊標(biāo)題進(jìn)入)
lonza 無血清培養(yǎng)基 (點(diǎn)擊標(biāo)題進(jìn)入)
基因修飾T細(xì)胞因可幫助人體免疫系統(tǒng)識(shí)別并攻擊腫瘤����,為此被稱為腫瘤治療的"第五支柱"�。
上述治療方法已經(jīng)在血癌����,如白血病中顯示出治療功效。在某些腫瘤類型如間皮瘤治療過程中���,當(dāng)這些“修修補(bǔ)補(bǔ)”的T細(xì)胞被再注入到患者血液中時(shí)���,患者腫瘤會(huì)很好抵抗T細(xì)胞攻擊。
研究人員試圖直接向腫瘤區(qū)域提供基因修飾后的T細(xì)胞�����,并發(fā)現(xiàn)這些T細(xì)胞不僅攻擊了癌細(xì)胞��,同時(shí)成功阻斷了癌癥再次發(fā)生�����。他們的研究結(jié)果發(fā)表在Science Translational Medicine雜志上��。
該研究主要使用人源T細(xì)胞和小鼠腫瘤����,其研究結(jié)果有助于加快開展1期臨床試驗(yàn)。研究人員嘗試了兩種靜脈注射����,將重新裝備(基因修飾)的T細(xì)胞注射入間皮瘤小鼠胸膜腔。奇怪的是��,當(dāng)基因修飾的T細(xì)胞到達(dá)腫瘤部位���,它們能“看到”敵人(癌細(xì)胞)��,激活自己的同時(shí)也激活其他T細(xì)胞��。
十多年來�����,研究人員已經(jīng)嘗試了基因改變T細(xì)胞使其產(chǎn)生受體����,以匹配腫瘤細(xì)胞的抗原��。上個(gè)月�,研究人員在費(fèi)城兒童醫(yī)院報(bào)道,當(dāng)患者的T細(xì)胞進(jìn)行基因修飾并重新引入患者體內(nèi)后,30名晚期復(fù)發(fā)的白血病患者中有27名患者經(jīng)歷緩解期�。
原文鏈接地址:
http://news.bioon.com/article/6661953.html
英文版
Regional delivery of mesothelin-targeted CAR T cell therapy generates potent and long-lasting CD4-dependent tumor immunity.
Adusumilli PS,et al.
Translating the recent success of chimeric antigen receptor (CAR) T cell therapy for hematological malignancies to solid tumors will necessitate overcoming several obstacles, including inefficient T cell tumor infiltration and insufficient functional persistence. Taking advantage of an orthotopic model that faithfully mimics human pleural malignancy, we evaluated two routes of administration of mesothelin-targeted T cells using the M28z CAR. We found that intrapleurally administered CAR T cells vastly outperformed systemically infused T cells, requiring 30-fold fewer M28z T cells to induce long-term complete remissions. After intrapleural T cell administration, prompt in vivo antigen-induced T cell activation allowed robust CAR T cell expansion and effector differentiation, resulting in enhanced antitumor efficacy and functional T cell persistence for 200 days. Regional T cell administration also promoted efficient elimination of extrathoracic tumor sites. This therapeutic efficacy was dependent on early CD4(+) T cell activation associated with a higher intratumoral CD4/CD8 cell ratios and CD28-dependent CD4(+) T cell-mediated cytotoxicity. In contrast, intravenously delivered CAR T cells, even when accumulated at equivalent numbers in the pleural tumor, did not achieve comparable activation, tumor eradication, or persistence. The ability of intrapleurally administered T cells to circulate and persist supports the concept of delivering optimal CAR T cell therapy through "regional distribution centers." On the basis of these results, we are opening a phase 1 clinical trial to evaluate the safety of intrapleural administration of mesothelin-targeted CAR T cells in patients with primary or secondary pleural malignancies.
細(xì)胞治療使用的 lonza 04-418Q 無血清培養(yǎng)基 (點(diǎn)擊標(biāo)題進(jìn)入)
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