IMMUNOLOGICAL TARGETS OF HIV-INFECTION - T-CELLS

被引：10

作者：

SHEARER, WT

ROSENBLATT, HM

SCHLUCHTER, MD

MOFENSON, LM

DENNY, TN

WILLOUGHBY, A

NUGENT, R

MOYE, J

BERENDES, HW

RIGAPEREZ, JG

DURAKO, S

JORDAN, C

HIRSCHHORN, R

BETHEL, J

SHAH, K

CHOW, J

EDELSON, P

SANDERS, D

BONAGURA, V

VALACER, D

HENLEY, W

BAMJI, M

GUPTA, A

LI, KI

ABRAMS, EJ

FIKRIG, S

BAKSHI, SS

PAHWA, S

KRASINSKI, K

PITT, J

BERNSTEIN, L

RUBINSTEIN, A

JOHNSON, G

COOPER, ER

FRENKEL, L

LISCHNER, HW

RAPHAEL, SA

JOHNSON, JP

RAKUSAN, T

NESHEIM, S

NAHMIAS, A

KEYSERLING, H

YOGEV, R

CHADWICK, E

RICH, K

GUERRAHANSON, IC

PETRU, A

DIAZ, C

SANTINI, JLC

JIMENEZ, E

机构：

[1] UNIV TEXAS, BAYLOR COLL MED, SCH MED, DEPT PEDIAT, HOUSTON, TX 77030 USA

[2] BAYLOR COLL MED, DEPT MICROBIOL, HOUSTON, TX 77030 USA

[3] BAYLOR COLL MED, DEPT IMMUNOL, HOUSTON, TX 77030 USA

[4] CLEVELAND CLIN FDN, DEPT BIOSTAT EPIDEMIOL, CLEVELAND, OH 44195 USA

[5] NICHHD, ROCKVILLE, MD 20892 USA

[6] UNIV MED & DENT NEW JERSEY, DEPT PEDIAT, NEWARK, NJ 07103 USA

[7] CHILDRENS HOSP NEW JERSEY, NEWARK, NJ 07103 USA

[8] NICHHD, PEDIAT ADOLESCENT & MATERNAL AIDS BRANCH, BETHESDA, MD USA

[9] NICHHD, DIV PREVENT RES, BETHESDA, MD 20892 USA

[10] WESTAT CORP, ROCKVILLE, MD USA

[11] LINCOLN HOSP CTR, BRONX, NY USA

[12] NEW YORK HOSP, CORNELL MED CTR, NEW YORK, NY USA

[13] SCHNEIDER CHILDRENS HOSP, LONG ISL JEWISH MED CTR, QUEENS HOSP CTR, NEW HYDE PK, NY 11042 USA

[14] BETH ISRAEL MED CTR, NEW YORK, NY USA

[15] METROPOLITAN HOSP CTR, NEW YORK, NY USA

[16] NEW YORK MED COLL, VALHALLA, NY USA

[17] HARLEM HOSP MED CTR, NEW YORK, NY USA

[18] SUNY HLTH SCI CTR, BROOKLYN, NY USA

[19] ST LUKES ROOSEVELT HOSP, NEW YORK, NY USA

[20] N SHORE UNIV HOSP, MANHASSET, NY USA

[21] NYU, BELLEVUE HOSP CTR, MED CTR, NEW YORK, NY 10016 USA

[22] BABIES HOSP, NEW YORK, NY USA

[23] ALBERT EINSTEIN COLL MED, BRONX, NY USA

[24] UNIV CONNECTICUT, CTR HLTH, HARTFORD, CT USA

[25] BOSTON CITY HOSP, BOSTON, MA USA

[26] UNIV MED & DENT NEW JERSEY, ROBERT WOOD JOHNSON MED SCH, NEW BRUNSWICK, NJ USA

[27] ST CHRISTOPHERS HOSP, PHILADELPHIA, PA USA

[28] UNIV MARYLAND, BALTIMORE, MD USA

[29] CHILDRENS HOSP, NATL MED CTR, WASHINGTON, DC 20010 USA

[30] EMORY UNIV, SCH MED, ATLANTA, GA USA

[31] CHILDRENS MEM HOSP, CHICAGO, IL USA

[32] UNIV ILLINOIS, COLL MED, CHICAGO, IL USA

[33] CHILDRENS HOSP, MED CTR, OAKLAND, CA USA

[34] UNIV PUERTO RICO, SAN JUAN, PR USA

[35] SAN JUAN CITY HOSP, SAN JUAN, PR USA

[36] RAMON RUIZ ARNAU UNIV HOSP, BAYAMON, PR USA

[37] MILES INC, CUTTER BIOL, BERKELEY, CA 94701 USA

[38] NHLBI, BETHESDA, MD USA

[39] CASE WESTERN RESERVE UNIV, CLEVELAND, OH USA

[40] HARVARD UNIV, CHILDRENS HOSP, SCH MED, BOSTON, MA 02115 USA

[41] MT SINAI SCH MED, NEW YORK, NY USA

[42] COLUMBIA UNIV, PRESBYTERIAN HOSP CITY NEW YORK, NEW YORK, NY USA

[43] UNIV CALIF LOS ANGELES, SCH MED, LOS ANGELES, CA USA

[44] UNIV TEXAS, HLTH SCI CTR, SAN ANTONIO, TX USA

来源：

PEDIATRIC AIDS: CLINICAL, PATHOLOGIC, AND BASIC SCIENCE PERSPECTIVES | 1993年 / 693卷

关键词：

D O I：

10.1111/j.1749-6632.1993.tb26255.x

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

One of the principal targets of HIV infection is the human peripheral blood CD4+ T cell, resulting in progressive CD4+ lymphocyte loss. Hypothesized mechanisms for this loss include apoptosis, cytolytic reactions, V-p gene deletion of the T-cell receptor (TCR) by superantigens, CD4+ lymphocyte syncytium formation, and autoimmune reactions. In adults with HIV infection, the critical decline in CD4+ lymphocyte number that heralds the onset of AIDS-defining conditions is well characterized, whereas in infants and children the critical level of CD4+ cells predisposing to the development of AIDS-defining conditions or mortality is not fully characterized, due to an incomplete knowledge of CD4+ lymphocyte number and changes with age in normal and HIV-infected children. In a prospective study of 317 infants born to HIV-infected women, early results show that the monthly change in absolute CD4+ lymphocyte number over a 3- to 9-month period in HIV-infected infants was - 109 cells/mm3 per month, at least double the rate of decline measured in HIV-noninfected infants in the study or that calculated from normal infants' values reported in the literature. In other clinical studies in HIV-infected infants and children, it was possible to study the effect of low CD4+ cell counts on clinical status and mortality. In HIV-infected pediatric patients younger than 1 year, it was possible to correlate low CD4+ cell number with advanced disease status (CDC pediatric class P-2). It was also possible to correlate extremely low CD4+ cell counts (<200 cells/mm3) in HIV-infected children with a significant risk of mortality within the next 3 months of life. Sequential CD4+ cell analysis of HlV-high-risk infants will delineate the rate of HIV-related decline in CD4+ cells, thus facilitating the diagnosis of HIV infection and aiding in identification of HIV-infected children at high risk of disease progression or death.

引用

页码：35 / 51

页数：17

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