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在感染人型支原体、肺炎支原体和解脲脲原体的黑猩猩身上进行实验性诱导的脓毒性关节炎。

Experimentally induced septic arthritis in chimpanzees infected with Mycoplasma hominis, Mycoplasma pneumoniae, and Ureaplasma urealyticum.

作者信息

Barile M F, Kapatais-Zoumbos K, Snoy P, Grabowski M W, Sneller M, Miller L, Chandler D K

机构信息

Laboratory of Mycoplasma, Food and Drug Administration, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland.

出版信息

Clin Infect Dis. 1994 May;18(5):694-703. doi: 10.1093/clinids/18.5.694.

Abstract

Mycoplasma hominis was isolated in pure culture from septic synovial aspirates from an individual (patient A) during 16 different bouts of exacerbation over a 70-month period of observation. Two isolates, 10(7) and also 10(6) color-changing units (CCU) of the 1620 isolate and 5 x 10(4) CCU of the 1628 isolate, caused inflammation in chimpanzees inoculated intraarticularly. Inflammation was also induced with 10(7) CCU of the 2010B isolate, serovar VII of Ureaplasma urealyticum, recovered from an agammaglobulinemic individual (patient B) with septic polyarthritis and with 3 x 10(6) CCU of the PI-1428 isolate of Mycoplasma pneumoniae. Inflammation persisted for up to 36 days and was self-limiting. The aspirates contained up to 220,000 white blood cells/mm3 and up to 10(7) CCU/mL. There was good correlation between the severity of inflammation and the numbers of organisms, but antibody was not detected in aspirates during the peak severity of disease. As the numbers of organisms, decreased, detectable levels of antibody increased, thus suggesting that antibody may have been bound to antigen. Chimpanzees previously infected with either the 1628 isolate of M. hominis or the 2010B isolate of U. urealyticum were protected on challenge with > 100 times the minimal dose causing arthritis. Chimpanzees showed little or no inflammation when inoculated intraarticularly with 5 x 10(8) CCU of the type strain PG-21 of M. hominis or with the type strain CO of U. urealyticum or when inoculated intravenously with 3 x 10(8) CCU of the arthrogenic 1620 isolate of M. hominis.

摘要

在70个月的观察期内,从一名个体(患者A)的16次不同发作的化脓性滑膜炎抽出液中分离出了纯培养的人型支原体。1620株的两个分离株,10(7)以及10(6)个变色单位(CCU),和1628株的5×10(4) CCU,经关节内接种可在黑猩猩中引起炎症。从一名患有化脓性多关节炎的无丙种球蛋白血症个体(患者B)中分离出的解脲脲原体血清型VII的2010B株的10(7) CCU,以及肺炎支原体的PI - 1428株的3×10(6) CCU也可诱导炎症。炎症持续长达36天,且具有自限性。抽出液中白细胞计数高达220,000个/mm3,支原体数量高达10(7) CCU/mL。炎症严重程度与病原体数量之间存在良好的相关性,但在疾病严重程度峰值期间,抽出液中未检测到抗体。随着病原体数量减少,可检测到的抗体水平升高,因此提示抗体可能已与抗原结合。先前感染过人型支原体1628株或解脲脲原体2010B株的黑猩猩,在接受超过引起关节炎的最小剂量100倍的攻击时受到保护。当关节内接种人型支原体标准株PG - 21的5×10(8) CCU或解脲脲原体标准株CO,或静脉内接种人型支原体致关节炎的1620株的3×10(8) CCU时,黑猩猩几乎没有或没有炎症反应。

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