CAR T Cells Targeting B7-H3, a Pan-Cancer Antigen, Demonstrate Potent Preclinical Activity Against Pediatric Solid Tumors and Brain Tumors

Majzner Robbie G.; Theruvath Johanna L.; Nellan Anandani; Heitzeneder Sabine; Cui Yongzhi; Mount Christopher W.; Rietberg Skyler P.; Linde Miles H.; Xu Peng; Rota Christopher; Sotillo Elena; Labanieh Louai; Lee Daniel W.; Orentas Rimas J.; Dimitrov Dimiter S.; Zhu Zhongyu; St Croix Brad; Delaidelli Alberto; Sekunova Alla; Bonvini Ezio; Mitra Siddhartha S.; Quezado Martha M.; Majeti Ravindra; Monje Michelle; Sorensen Poul H. B.; Maris John M.; Mackall Crystal L.

首页> 外文期刊>Clinical cancer research: an official journal of the American Association for Cancer Research >CAR T Cells Targeting B7-H3, a Pan-Cancer Antigen, Demonstrate Potent Preclinical Activity Against Pediatric Solid Tumors and Brain Tumors

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CAR T Cells Targeting B7-H3, a Pan-Cancer Antigen, Demonstrate Potent Preclinical Activity Against Pediatric Solid Tumors and Brain Tumors

机译：靶向B7-H3的CAR T细胞，泛癌抗原，证明了对儿科实体肿瘤和脑肿瘤的有效的临床前活性

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Purpose: Patients with relapsed pediatric solid tumors and CNS malignancies have few therapeutic options and frequently die of their disease. Chimeric antigen receptor (CAR) T cells have shown tremendous success in treating relapsed pediatric acute lymphoblastic leukemia, but this has not yet translated to treating solid tumors. This is partially due to a paucity of differentially expressed cell surface molecules on solid tumors that can be safely targeted. Here, we present B7-H3 (CD276) as a putative target for CAR T-cell therapy of pediatric solid tumors, including those arising in the central nervous system.

机译：目的：复发的小儿实体肿瘤和CNS恶性肿瘤的患者有很少的治疗选择，并且经常死于疾病。嵌合抗原受体（轿厢）T细胞表现出巨大成功处理复发的小儿急性淋巴细胞白血病，但这尚未翻译成治疗实体肿瘤。这部分是由于可以安全靶向的固体瘤上的差异表达细胞表面分子的缺乏。在这里，我们将B7-H3（CD276）作为足部固体肿瘤的汽车T细胞治疗的推定靶标，包括中枢神经系统中产生的靶标。

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来源
《Clinical cancer research: an official journal of the American Association for Cancer Research》 |2019年第8期|共15页
作者
Majzner Robbie G.; Theruvath Johanna L.; Nellan Anandani; Heitzeneder Sabine; Cui Yongzhi; Mount Christopher W.; Rietberg Skyler P.; Linde Miles H.; Xu Peng; Rota Christopher; Sotillo Elena; Labanieh Louai; Lee Daniel W.; Orentas Rimas J.; Dimitrov Dimiter S.; Zhu Zhongyu; St Croix Brad; Delaidelli Alberto; Sekunova Alla; Bonvini Ezio; Mitra Siddhartha S.; Quezado Martha M.; Majeti Ravindra; Monje Michelle; Sorensen Poul H. B.; Maris John M.; Mackall Crystal L.;
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作者单位

Stanford Univ Sch Med Dept Pediat Palo Alto CA 94304 USA;

Stanford Univ Sch Med Dept Pediat Palo Alto CA 94304 USA;

Univ Colorado Dept Pediat Denver Anschutz Med Ctr Denver CO 80202 USA;

Stanford Univ Sch Med Dept Pediat Palo Alto CA 94304 USA;

NCI Pediat Oncol Branch Bethesda MD 20892 USA;

Stanford Univ Sch Med Dept Neurol Palo Alto CA 94304 USA;

Stanford Univ Sch Med Dept Pediat Palo Alto CA 94304 USA;

Stanford Univ Sch Med Immunol Grad Program Palo Alto CA 94304 USA;

Stanford Univ Sch Med Dept Pediat Palo Alto CA 94304 USA;

NCI Pediat Oncol Branch Bethesda MD 20892 USA;

Stanford Univ Sch Med Dept Pediat Palo Alto CA 94304 USA;

Stanford Univ Sch Med Dept Bioengn Palo Alto CA 94304 USA;

Univ Virginia Div Pediat Hematol Oncol Dept Pediat Charlottesville VA USA;

Univ Washington Sch Med Dept Pediat Seattle WA 98195 USA;

Univ Pittsburgh Med Sch Ctr Antibody Therapeut Pittsburgh PA USA;

NCI Canc &

Inflammat Program NIH Frederick MD 21701 USA;

NCI Tumor Angiogenesis Unit MCGP NIH Frederick MD 21701 USA;

Univ British Columbia Dept Pathol &

Lab Med Vancouver BC Canada;

Univ British Columbia Dept Pathol &

Lab Med Vancouver BC Canada;

MacroGenics Inc Rockville MD USA;

Univ Colorado Dept Pediat Denver Anschutz Med Ctr Denver CO 80202 USA;

NCI Lab Pathol Ctr Canc Res NIH Bethesda MD 20892 USA;

Inst Stem Cell Biol &

Regenerat Med Palo Alto CA USA;

Stanford Univ Sch Med Dept Neurol Palo Alto CA 94304 USA;

Univ British Columbia Dept Pathol &

Lab Med Vancouver BC Canada;

Univ Penn Childrens Hosp Philadelphia Philadelphia PA 19104 USA;

Stanford Univ Sch Med Dept Pediat Palo Alto CA 94304 USA;

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正文语种 eng
中图分类肿瘤学;
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1. CAR T Cells Targeting B7-H3, a Pan-Cancer Antigen, Demonstrate Potent Preclinical Activity Against Pediatric Solid Tumors and Brain Tumors [J] . Majzner Robbie G., Theruvath Johanna L., Nellan Anandani, Clinical cancer research: an official journal of the American Association for Cancer Research . 2019,第8期

机译：靶向B7-H3的CAR T细胞，泛癌抗原，证明了对儿科实体肿瘤和脑肿瘤的有效的临床前活性
2. CAR T CELLS TARGETING B7-H3, A PAN-CANCER ANTIGEN, DEMONSTRATE POTENT PRECLINICAL ACTIVITY AGAINST PEDIATRIC SOLID TUMORS AND BRAIN TUMORS [J] . Majzner Robbie, Nellan Anandani, Heitzeneder Sabine, Pediatric blood & cancer . 2018,第Suppla1期

机译：靶向B7-H3的CAR T细胞，泛癌抗原，证明了对儿科实体肿瘤和脑肿瘤的有效的临床前活性
3. CAR T CELLS TARGETING B7-H3, A PAN-CANCER ANTIGEN, DEMONSTRATE POTENT PRECLINICAL ACTIVITY AGAINST PEDIATRIC SOLID TUMORS AND BRAIN TUMORS [J] . Majzner Robbie, Nellan Anandani, Heitzeneder Sabine, Pediatric blood & cancer . 2018,第Suppla1期

机译：靶向B7-H3的CAR T细胞，泛癌抗原，证明了对儿科实体肿瘤和脑肿瘤的有效的临床前活性
4. KTN0182A, an Anti-KIT, Pyrrolobenzodiazepine (PBD)-Containing Antibody Drug Conjugate (ADC) Demonstrates Potent Antitumor Activity In Vitro and In Vivo Against a Broad Range of Tumor Types [C] . Sergio Trombetta, Christine Lubeski, Gary C. Kemp, PEGS . 2015

机译：KTN0182A，抗试剂盒，吡咯唑二氮杂己酮（PBD）抗体药物缀合物（ADC）在体外和体内抗抗肿瘤类型的抗肿瘤活性
5. Targeting distinct tumor-infiltrating myeloid cells by inhibiting CSF-1 receptor in solid tumors. [D] . Priceman, Saul Jonathan. 2009

机译：通过抑制实体瘤中的CSF-1受体靶向不同的浸润肿瘤的骨髓细胞。
6. Tandem CAR-T cells targeting CD70 and B7-H3 exhibit potent preclinical activity against multiple solid tumors [O] . Meijia Yang, Xin Tang, Zongliang Zhang, 2020

机译：靶向CD70和B7-H3的串联CAR-T细胞对多种实体瘤表现出强大的临床前活性
7. Antitumor Responses in the Absence of Toxicity in Solid Tumors by Targeting B7-H3 Via Chimeric Antigen Receptor T Cells [O] . Hongwei Du, Koichi Hirabayashi, Sarah Ahn, 2018

机译：通过嵌合抗原受体T细胞靶向B7-H3，在实体瘤中没有毒性的抗肿瘤反应

CAR T Cells Targeting B7-H3, a Pan-Cancer Antigen, Demonstrate Potent Preclinical Activity Against Pediatric Solid Tumors and Brain Tumors

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