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| DOI | 10.1038/s41467-017-02235-3 |
| CXCR1-or CXCR2-modified CAR T cells co-opt IL-8 for maximal antitumor efficacy in solid tumors | |
| Jin, Linchun1; Tao, Haipeng2; Karachi, Aida1; Long, Yu1,2; Hou, Alicia Y.1; Na, Meng2; Dyson, Kyle A.1; Grippin, Adam J.1; Deleyrolle, Loic P.1,3; Zhang, Wang2; Rajon, Didier A.1,3; Wang, Qiong J.4,6; Yang, James C.4; Kresak, Jesse L.5; Sayour, Elias J.1,3; Rahman, Maryam1,3; Bova, Frank J.1,3; Lin, Zhiguo2; Mitchell, Duane A.1,3; Huang, Jianping1,3 | |
| 2019-09-05 | |
| 发表期刊 | NATURE COMMUNICATIONS
 |
| ISSN | 2041-1723 |
| 出版年 | 2019 |
| 卷号 | 10 |
| 文章类型 | Article |
| 语种 | 英语 |
| 国家 | USA; Peoples R China |
| 英文摘要 | Chimeric antigen receptor (CAR) T-cell therapy targeting solid tumors has stagnated as a result of tumor heterogeneity, immunosuppressive microenvironments, and inadequate intratumoral T cell trafficking and persistence. Early (<= 3 days) intratumoral presentation of CAR T cells post-treatment is a superior predictor of survival than peripheral persistence. Therefore, we have co-opted IL-8 release from tumors to enhance intratumoral T-cell trafficking through a CAR design for maximal antitumor activity in solid tumors. Here, we demonstrate that IL-8 receptor, CXCR1 or CXCR2, modified CARs markedly enhance migration and persistence of T cells in the tumor, which induce complete tumor regression and long-lasting immunologic memory in pre-clinical models of aggressive tumors such as glioblastoma, ovarian and pancreatic cancer. |
| 领域 | 资源环境 |
| 收录类别 | SCI-E |
| WOS记录号 | WOS:000483922400016 |
| WOS关键词 | CANCER REGRESSION ; IN-VIVO ; INTERLEUKIN-8 ; PERSISTENCE ; LYMPHOCYTES ; DIFFERENTIATION ; EXPRESSION ; INDUCTION ; MIGRATION ; MELANOMA |
| WOS类目 | Multidisciplinary Sciences |
| WOS研究方向 | Science & Technology - Other Topics |
| URL | 查看原文 |
| 引用统计 | |
| 文献类型 | 期刊论文 |
| 条目标识符 | http://119.78.100.173/C666/handle/2XK7JSWQ/203635 |
| 专题 | 资源环境科学 |
| 作者单位 | 1.Univ Florida, Lillian S Wells Dept Neurosurg, Gainesville, FL 32611 USA; 2.Harbin Med Univ, Sect 4, Dept Neurosurg, Affiliated Hosp 1, Harbin, Heilongjiang, Peoples R China; 3.Univ Florida, Preston A Wells Jr Ctr Brain Tumor Therapy, Gainesville, FL 32611 USA; 4.NCI, Surg Branch, Bldg 10, Bethesda, MD 20892 USA; 5.Univ Florida, Dept Pathol Immunol & Lab Med, Gainesville, FL USA; 6.Legend Biotech USA Inc, Gainesville, FL USA |
| 推荐引用方式 GB/T 7714 | Jin, Linchun,Tao, Haipeng,Karachi, Aida,et al. CXCR1-or CXCR2-modified CAR T cells co-opt IL-8 for maximal antitumor efficacy in solid tumors[J]. NATURE COMMUNICATIONS,2019,10. |
| APA | Jin, Linchun.,Tao, Haipeng.,Karachi, Aida.,Long, Yu.,Hou, Alicia Y..,...&Huang, Jianping.(2019).CXCR1-or CXCR2-modified CAR T cells co-opt IL-8 for maximal antitumor efficacy in solid tumors.NATURE COMMUNICATIONS,10. |
| MLA | Jin, Linchun,et al."CXCR1-or CXCR2-modified CAR T cells co-opt IL-8 for maximal antitumor efficacy in solid tumors".NATURE COMMUNICATIONS 10(2019). |
| 条目包含的文件 | 条目无相关文件。 | |||||
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