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在与高水平循环抗大肠杆菌内毒素核心抗体相关的铜绿假单胞菌败血症中生存率提高。

Enhanced survival in Pseudomonas aeruginosa septicemia associated with high levels of circulating antibody to Escherichia coli endotoxin core.

作者信息

Pollack M, Huang A I, Prescott R K, Young L S, Hunter K W, Cruess D F, Tsai C M

出版信息

J Clin Invest. 1983 Dec;72(6):1874-81. doi: 10.1172/JCI111150.

DOI:10.1172/JCI111150
PMID:6358257
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC437026/
Abstract

We studied the relationship between serum antibodies to the cross-reactive endotoxin core of Escherichia coli and survival following Pseudomonas aeruginosa septicemia. Core glycolipid was purified from the outer cell membrane of a uridine diphosphate galactose 4-epimerase-deficient rough mutant E. coli (J5 strain), characterized, and used as the antigen in a quantitative enzyme-linked immunosorbent assay (ELISA) to measure core-specific IgG and IgM antibodies. 43 patients with Pseudomonas septicemia, among whom there was a mortality of 42%, were evaluated. Core-specific antibody concentrations in acute sera ranged from 1 to 49 micrograms/ml in the case of IgG and from 1 to 200 micrograms/ml for IgM. Core-specific antibodies of both isotypes were higher in patients who survived compared with those who succumbed to their septicemias (mean, microgram/ml +/- SEM, 26 +/- 3 vs. 14 +/- 4, P = 0.005 for IgG, and 55 +/- 12 vs. 18 +/- 5, P = 0.009 for IgM). Although total IgG levels were also higher in acute sera from survivors compared with nonsurvivors (mean, mg/dl +/- SEM, 1,120 +/- 99 vs. 694 +/- 119, P = 0.004), total IgM levels were virtually identical in the two groups (146 +/- 23 vs. 148 +/- 48, P = 0.52). Conversely, patients with core-specific IgG levels greater than 10 micrograms/ml at the onset of septicemia had better survival than those with levels less than 10 micrograms/ml (79 vs. 14%, P less than 0.001), and patients with core-specific IgM levels greater than 30 micrograms/ml had better survival than those with levels less than 30 micrograms/ml (81 vs. 44%, P = 0.01). In comparison, patients with total IgG levels greater than 1,000 mg/dl also had better survival than those with levels less than 1,000 mg/dl (82 vs. 42%, P = 0.01), while those with total IgM levels greater than 150 mg/dl showed somewhat less improvement in survival compared with those with levels less than 150 mg/dl (71 vs. 50%, P = 0.12). Core-specific IgM was highly correlated with core-specific IgG (r = 0.52), but not with type-specific anti-lipopolysaccharide (r = 0.13) or anti-toxin A (r = 0.12) antibodies, or with total IgG (r = 0.28) or IgM (r = 0.31). In contrast, core-specific IgG correlated somewhat more closely with type-specific antibodies (r = 0.36), and with total IgG (r = 0.51) and IgM (r = 0.52). Stepwise linear discriminant analysis indicated that type-specific antibody levels were the best predictor of outcome, among those antibodies examined, followed by anti-core IgM. Although anti-core IgG, anti-toxin A, and total IgG levels all correlated individually with survival, none augmented the prognostic power of type-specific antibodies in combination with anti-core IgM, which together predicted outcome accurately 73.5% of the time. Host factors not significantly associated with anti-core antibody levels included rapidly fatal underlying disease, age, sex, leukopenia, and prior treatment with cytotoxic drugs. In contrast, prior steroid therapy was associated with low levels of both core-specific IgG and IgM (P < 0.05). These data suggest cross-protective activity against P. aeruginosa septicemia of naturally occurring antibodies to the endotoxin core of E. coli. Anti-core antibodies, particularly of the IgM isotype appear to augment the more specific protective immunity engendered by antibodies to the O-specific side chains of Pseudomonas lipopolysaccharides. This cross-protective immunity likely applies to other Gram-negative pathogens as well.

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0273/437026/c5c4eee682cd/jcinvest00155-0024-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0273/437026/c5c4eee682cd/jcinvest00155-0024-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0273/437026/c5c4eee682cd/jcinvest00155-0024-a.jpg
摘要

我们研究了针对大肠杆菌交叉反应性内毒素核心的血清抗体与铜绿假单胞菌败血症后生存率之间的关系。从尿苷二磷酸半乳糖4-表异构酶缺陷的粗糙突变型大肠杆菌(J5菌株)的外细胞膜中纯化核心糖脂,对其进行表征,并将其用作定量酶联免疫吸附测定(ELISA)中的抗原,以测量核心特异性IgG和IgM抗体。对43例铜绿假单胞菌败血症患者进行了评估,其中死亡率为42%。急性血清中核心特异性抗体浓度,IgG为1至49微克/毫升,IgM为1至200微克/毫升。与死于败血症的患者相比,存活患者的两种同型核心特异性抗体水平更高(平均值,微克/毫升±标准误,IgG为26±3对14±4,P = 0.005;IgM为55±12对18±5,P = 0.009)。尽管存活患者急性血清中的总IgG水平也高于非存活患者(平均值,毫克/分升±标准误,1120±99对694±119,P = 0.004),但两组的总IgM水平实际上相同(146±23对148±48,P = 0.52)。相反,败血症发作时核心特异性IgG水平大于10微克/毫升的患者比水平低于10微克/毫升的患者生存率更高(79%对14%,P<0.001),核心特异性IgM水平大于30微克/毫升的患者比水平低于30微克/毫升的患者生存率更高(81%对44%,P = 0.01)。相比之下,总IgG水平大于1000毫克/分升的患者也比水平低于1000毫克/分升的患者生存率更高(82%对42%,P = 0.01),而总IgM水平大于150毫克/分升的患者与水平低于150毫克/分升的患者相比,生存率的改善程度略小(71%对50%,P = 0.12)。核心特异性IgM与核心特异性IgG高度相关(r = 0.52),但与型特异性抗脂多糖(r = 0.13)或抗毒素A(r = 0.12)抗体、总IgG(r = 0.28)或IgM(r = 0.31)均无相关性。相比之下,核心特异性IgG与型特异性抗体(r = 0.36)、总IgG(r = 0.51)和IgM(r = 0.52)的相关性稍强。逐步线性判别分析表明,在所检测的抗体中,型特异性抗体水平是预后的最佳预测指标,其次是抗核心IgM。尽管抗核心IgG、抗毒素A和总IgG水平均与生存率单独相关,但它们与型特异性抗体和抗核心IgM联合使用时,均未增强其预后预测能力,二者联合可准确预测73.5%的预后情况。与抗核心抗体水平无显著相关性的宿主因素包括快速致命的基础疾病、年龄、性别、白细胞减少以及先前使用细胞毒性药物治疗。相反,先前的类固醇治疗与核心特异性IgG和IgM水平较低相关(P<0.05)。这些数据表明,针对大肠杆菌内毒素核心的天然抗体对铜绿假单胞菌败血症具有交叉保护活性。抗核心抗体,尤其是IgM同型抗体,似乎增强了由针对铜绿假单胞菌脂多糖O-特异性侧链的抗体所产生的更具特异性的保护性免疫。这种交叉保护性免疫可能也适用于其他革兰氏阴性病原体。

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