APOPTOSIS PARALLELS LYMPHOPOIESIS IN BONE-MARROW TRANSPLANTATION AND HIV DISEASE

被引：23

作者：

DONNENBERG, AD

MARGOLICK, JB

BELTZ, LA

DONNENBERG, VS

RINALDO, CR

机构：

[1] JOHNS HOPKINS UNIV, SCH HYG & PUBL HLTH, BALTIMORE, MD USA

[2] UNIV PITTSBURGH, GRAD SCH PUBL HLTH, PITTSBURGH, PA USA

来源：

RESEARCH IN IMMUNOLOGY | 1995年 / 146卷 / 01期

关键词：

APOPTOSIS; LYMPHOPOIESIS; AIDS; HIV; BONE MARROW; TRANSPLANTATION; TOLERANCE; FLOW CYTOMETRY;

D O I：

10.1016/0923-2494(96)80236-7

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Apoptosis has been implicated in a variety of physiological processes ranging from tissue modeling to deletion of autoreactive T lymphocytes during thymic development. The recent finding that a large proportion of peripheral T cells from HIV-infected subjets apoptose in culture raises an important issue: does this represent a pathologic mechanism by which the virus disrupts the immune system, or a normal physiologic response to virus-mediated T-cell loss? To study the potential relationship between apoptosis and lymphopoiesis, we compared apoptosis rates in unstimulated lymphocyte cultures from healthy subjets, HIV+ gay men, and bone marrow transplant (BMT) recipients undergoing immune reconstitution. BMT recipients were chosen because they undergo massive regeneration of lymphocytes following marrow ablation and graft infusion. The data obtained in BMT recipients suggests that elevated apoptosis accompanies, and is the consequence of, elevated lymphopoiesis. We also found a strong inverse relationship between in vitro T-cell apoptosis rates and peripheral T-cell counts. These results provide a new interpretation for elevated apoptosis observed in HIV-infected individuals - that it reflects increased T-cell turnover consequent to virus-mediated destruction of CD4(+) T cells.

引用

页码：11 / 21

页数：11

共 27 条

[1]

ADLEMAN LM, 1993, J ACQ IMMUN DEF SYND, V6, P144

[2]

AMEISEN JC, 1992, CR ACAD SCI III-VIE, V314, P47

[3] CROSS-LINKING CD4 BY HUMAN IMMUNODEFICIENCY VIRUS-GP120 PRIMES T-CELLS FOR ACTIVATION-INDUCED APOPTOSIS [J].

BANDA, NK ;

BERNIER, J ;

KURAHARA, DK ;

KURRLE, R ;

HAIGWOOD, N ;

SEKALY, RP ;

FINKEL, TH .

JOURNAL OF EXPERIMENTAL MEDICINE, 1992, 176 (04) :1099-1106

[4] BCL-X, A BCL-2-RELATED GENE THAT FUNCTIONS AS A DOMINANT REGULATOR OF APOPTOTIC CELL-DEATH [J].

BOISE, LH ;

GONZALEZGARCIA, M ;

POSTEMA, CE ;

DING, LY ;

LINDSTEN, T ;

TURKA, LA ;

MAO, XH ;

NUNEZ, G ;

THOMPSON, CB .

CELL, 1993, 74 (04) :597-608

[5]

DONNENBERG AD, 1987, TRANSPLANT P, V19, P144

[6]

DONNENBERG AD, 1993, C APOPTOSIS AIDS CAN, P138

[7]

DONNENBERG AD, 1995, IN PRESS CLIN IMMUNO

[8]

GOUGEON ML, 1991, CR ACAD SCI III-VIE, V312, P529

[9] PROGRAMMED CELL-DEATH IN AIDS-RELATED HIV AND SIV INFECTIONS [J].

GOUGEON, ML ;

GARCIA, S ;

HEENEY, J ;

TSCHOPP, R ;

LECOEUR, H ;

GUETARD, D ;

RAME, V ;

DAUGUET, C ;

MONTAGNIER, L .

AIDS RESEARCH AND HUMAN RETROVIRUSES, 1993, 9 (06) :553-563

[10] APOPTOSIS IN AIDS [J].

GOUGEON, ML ;

MONTAGNIER, L .

SCIENCE, 1993, 260 (5112) :1269-1270

← 1 2 3 →