AUTOREACTIVE T-CELL AND B-CELL RESPONDING TO MYELIN PROTEOLIPID PROTEIN IN MULTIPLE-SCLEROSIS AND CONTROLS

被引：226

作者：

SUN, JP

OLSSON, T

WANG, WZ

XIAO, BG

KOSTULAS, V

FREDRIKSON, S

EKRE, HP

LINK, H

机构：

[1] HUDDINGE UNIV HOSP,KAROLINSKA INST,DEPT NEUROL,S-14186 HUDDINGE,SWEDEN

[2] KABI BIOPHARMA,STOCKHOLM,SWEDEN

来源：

EUROPEAN JOURNAL OF IMMUNOLOGY | 1991年 / 21卷 / 06期

关键词：

D O I：

10.1002/eji.1830210620

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

The pathogenesis of multiple sclerosis (MS) could involve an autoimmune response to proteolipid protein (PLP). Immunization of experimental animals with this major myelin protein can lead to experimental allergic encephalomyelitis. To identify a possible role of PLP as target antigen in MS, we evaluated T cell immunity to PLP in blood and cerebrospinal fluid (CSF) from patients with MS and controls by counting cells which in response to PLP in short-term cultures secreted interferon-gamma. The PLP-specific B cell response was analyzed by counting cells secreting anti-PLP antibodies. PLP-reactive T cells were detected in blood of most MS patients (mean value 1 per 20 408 mononuclear cells), and at 41-fold higher numbers in CSF (mean 1 per 500 CSF cells). Anti-PLP IgG antibody-secreting cells were detected in blood from most MS patients (mean 1 per 30 303 cells), but such cells were 49-fold more frequent in CSF (mean 1 per 625 cells). PLP-reactive T and B cells were also detected in blood and CSF from control patients, but at much lower numbers. A strong and persistent autoimmune response to PLP as well as to other myelin proteins, enriched in CSF, is proposed to be pathogenetically important in MS.

引用

页码：1461 / 1468

页数：8

共 50 条

[31] MYELIN BASIC-PROTEIN AND PROTEOLIPID PROTEIN REACTIVITY OF BRAIN-DERIVED AND CEREBROSPINAL FLUID-DERIVED T-CELL CLONES IN MULTIPLE-SCLEROSIS AND POSTINFECTIOUS ENCEPHALOMYELITIS
HAFLER, DA
BENJAMIN, DS
BURKS, J
WEINER, HL
JOURNAL OF IMMUNOLOGY, 1987, 139 (01): : 68 - 72
[32] B-CELL ABNORMALITIES IN MULTIPLE-SCLEROSIS - A HYPOTHESIS
ROOS, RP
ARCHIVES OF NEUROLOGY, 1985, 42 (01) : 73 - 75
[33] CHANGES OF THE T-CELL POPULATIONS IN MULTIPLE-SCLEROSIS
SLUGA, E
SOUKUP, W
LISCHKA, K
WIENER KLINISCHE WOCHENSCHRIFT, 1983, 95 (16) : 598 - 598
[34] T-CELL RECEPTOR USE IN MULTIPLE-SCLEROSIS
UTZ, U
MARTIN, R
BROOKS, JA
BIDDISON, WE
MCFARLAND, HF
T-CELL RECEPTOR USE IN HUMAN AUTOIMMUNE DISEASES, 1995, 756 : 259 - 264
[35] T-CELL RECEPTOR BIOLOGY AND MULTIPLE-SCLEROSIS
LAUER, K
ANNALS OF NEUROLOGY, 1991, 30 (04) : 623 - 624
[36] T-CELL PHENOTYPE AND FUNCTION IN MULTIPLE-SCLEROSIS
HUGHES, PJ
COMPSTON, DAS
JOURNAL OF NEUROLOGY NEUROSURGERY AND PSYCHIATRY, 1988, 51 (05): : 735 - 735
[37] T-CELL SPECIFICITY AND CLONALITY IN MULTIPLE-SCLEROSIS
BACH, MA
RESEARCH IN IMMUNOLOGY, 1989, 140 (02): : 216 - 219
[38] MAJOR T-CELL RESPONSES IN MULTIPLE-SCLEROSIS
STEINMAN, L
WAISMAN, A
ALTMANN, D
MOLECULAR MEDICINE TODAY, 1995, 1 (02): : 79 - 83
[39] T-CELL SUBPOPULATION DEFICIENCY IN MULTIPLE-SCLEROSIS
CIONGOLI, AK
ALBERTINI, RD
MACPHERSON, B
HORNER, S
FAIRBANKS, T
ANNALS OF NEUROLOGY, 1977, 1 (05) : 500 - 500
[40] CHANGES IN T-CELL SUBPOPULATIONS IN MULTIPLE-SCLEROSIS
ACHIRON, A
MENDEL, M
RECHAVI, G
RAMOT, B
MELAMED, E
ANNALS OF NEUROLOGY, 1989, 26 (02) : 291 - 292

← 1 2 3 4 5 →