ANTIGEN-DRIVEN LONG TERM-CULTURED T-CELLS PROLIFERATE INVIVO, DISTRIBUTE WIDELY, MEDIATE SPECIFIC TUMOR-THERAPY, AND PERSIST LONG-TERM AS FUNCTIONAL MEMORY T-CELLS

被引：108

作者：

CHEEVER, MA

THOMPSON, DB

KLARNET, JP

GREENBERG, PD

机构：

[1] UNIV WASHINGTON, DEPT MED, DIV ONCOL, SEATTLE, WA 98195 USA

[2] UNIV WASHINGTON, DEPT MICROBIOL IMMUNOL, SEATTLE, WA 98195 USA

[3] FRED HUTCHINSON CANC RES CTR, SEATTLE, WA 98104 USA

来源：

JOURNAL OF EXPERIMENTAL MEDICINE | 1986年 / 163卷 / 05期

关键词：

D O I：

10.1084/jem.163.5.1100

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Mice bearing disseminated syngeneic FBL-3 leukemia were treated with cyclophosphamide plus long term-cultured T cells immune to FBL-3. The cultured T cells for therapy had been induced to grow in vitro for 62 d by intermittent stimulation with irradiated FBL-3. At the time of therapy, such antigen-driven long term-cultured T cells were greatly expanded in number, proliferated in vitro in response to FBL-3, and were specifically cytotoxic. Following adoptive transfer, donor T cells persisting in the host were identified and counted using donor and host mice congenic for the T cell marker Thy-1. The results show that antigen-driven long term-cultured T cells proliferated rapidly in vivo, distributed widely in host lymphoid organs, and were effective in tumor therapy. Moreover, the already rapid in vivo growth rate of donor T cells could be augmented by administration of exogenous IL-2. When cured mice were examined 120 d after therapy, donor L3T4+ T cells and donor Lyt-2+ T cells could be found in large numbers in host ascites, spleen, and mesenteric and axillary lymph nodes. The persisting donor T cells proliferated in vitro, and became specifically cytotoxic in response to FBL-3, demonstrating that antigen-driven long term-cultured T cells can persist long term in vivo and provide immunologic memory.

引用

页码：1100 / 1112

页数：13

共 41 条

[1] CLONES OF HELPER T-CELLS MEDIATE ANTIGEN-SPECIFIC, H-2-RESTRICTED DTH
BIANCHI, ATJ
HOOIJKAAS, H
BENNER, R
TEES, R
NORDIN, AA
SCHREIER, MH
[J]. NATURE, 1981, 290 (5801) : 62 - 63
[2] STUDIES ON CHEMICALLY-INDUCED RAT-TUMORS .2. PARTIAL PROTECTION AGAINST SYNGENEIC LETHAL TUMORS BY CLONED SYNGENEIC CYTO-TOXIC LYMPHOCYTES-T
BINZ, H
FENNER, M
ENGEL, R
WIGZELL, H
[J]. INTERNATIONAL JOURNAL OF CANCER, 1983, 32 (04) : 491 - 500
[3] BIOLOGY OF CLONED CYTO-TOXIC LYMPHOCYTES-T SPECIFIC FOR LYMPHOCYTIC CHORIOMENINGITIS VIRUS - CLEARANCE OF VIRUS INVIVO
BYRNE, JA
OLDSTONE, MBA
[J]. JOURNAL OF VIROLOGY, 1984, 51 (03) : 682 - 686
[4] INVIVO LOCALIZATION OF CLONED IL-2-DEPENDENT T-CELLS
CARROLL, AM
PALLADINO, MA
OETTGEN, H
DESOUSA, M
[J]. CELLULAR IMMUNOLOGY, 1983, 76 (01) : 69 - 80
[5] AUGMENTATION OF THE ANTI-TUMOR THERAPEUTIC EFFICACY OF LONG-TERM CULTURED LYMPHOCYTES-T BY INVIVO ADMINISTRATION OF PURIFIED INTERLEUKIN-2
CHEEVER, MA
GREENBERG, PD
FEFER, A
GILLIS, S
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1982, 155 (04) : 968 - 980
[6] CHEEVER MA, 1985, J IMMUNOL, V134, P3895
[7] CHEEVER MA, 1981, J IMMUNOL, V126, P1318
[8] CHEEVER MA, 1984, J IMMUNOL, V132, P2259
[9] CONTA BS, 1985, J IMMUNOL, V134, P2185
[10] DAILEY MO, 1985, J MOL CELL IMMUNOL, V2, P27

← 1 2 3 4 5 →