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Increased translocation of bacteria from the gastrointestinal tracts of tumor-bearing mice.

机译:荷瘤小鼠胃肠道细菌的移位增加。

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摘要

Aerobic gram-negative bacilli and other indigenous gastrointestinal (GI) bacteria are important opportunistic pathogens in immunosuppressed cancer patients. These same bacteria frequently translocate from the GI tracts of mice immunosuppressed by single injections of certain anticancer drugs or by T-lymphocyte impairments. Since similar cellular and humoral immune deficiencies may be present in the tumor-bearing host, we sought to determine if progressive growth of a tumor alone would be sufficient to enhance the translocation of indigenous bacteria from the murine GI tract. Pathogen-free DBA/2 mice were injected intraperitoneally with 10(6) viable sarcoma 180 (S-180) cells or 0.5 ml of sterile buffer. Mesenteric lymph nodes, livers, spleens, and kidneys were tested for the presence of translocated aerobic GI bacteria on various days after tumor injection. Immunity was assessed by measuring footpad delayed-type hypersensitivity and serum hemagglutinins to sheep erythrocytes. Overall, translocated aerobic GI bacteria infected 33 of 92 S-180-bearing mice (36%) and only 9 of 99 control mice (9%) (P less than 10(-6)). Cumulatively, 50 of 460 sites (10.9%) in S-180-bearing mice were infected with translocated GI bacteria as opposed to only 9 of 485 sites (1.9%) in control animals (P less than 10(-7)). GI bacteria often translocated to infect more than one site in tumor-bearing mice, but not in controls. Aerobic gram-negative bacilli translocated 11 times in tumor-bearing mice, but only once in controls, even though the mean cecal population levels of these bacteria were relatively low (range, 4.33 to 5.28 log10 bacteria per g). The population levels of cecal aerobic bacteria were similar in S-180 and control mice throughout the period of observation. S-180 mice had significantly suppressed (P less than 0.04) delayed-type hypersensitivity and serum hemagglutinin responses when sensitized 4 or 8 days after S-180 injection. S-180 growth was associated with a neutrophilic leukocytosis and a slight drop in platelet counts; no bleeding was detected. Thus, the translocation of gram-negative bacilli and other indigenous aerobic bacteria from the GI tract to the mesenteric lymph nodes and other organs was increased in immunosuppressed S-180-bearing mice, and this increase was not caused by bacterial overgrowth in the intestines or by neutropenia.
机译:有氧革兰氏阴性杆菌和其他本地胃肠道(GI)细菌是免疫抑制癌症患者的重要机会病原体。这些相同的细菌经常从单次注射某些抗癌药物或T淋巴细胞功能受损的小鼠的胃肠道中转移出来。由于在荷瘤宿主中可能存在类似的细胞和体液免疫缺陷,因此我们试图确定仅肿瘤的进行性生长是否足以增强本地细菌从鼠胃肠道的转运。将无病原体的DBA / 2小鼠腹膜内注射10(6)个存活肉瘤180(S-180)细胞或0.5 ml无菌缓冲液。在肿瘤注射后的不同天,检查肠系膜淋巴结,肝脏,脾脏和肾脏是否存在易位的好氧胃肠道细菌。通过测量脚垫延迟型超敏反应和对绵羊红细胞的血清血凝素评估免疫力。总体而言,易位的好氧胃肠道细菌感染了92只S-180小鼠中的33只(36%),而99只对照小鼠中只有9只(9%)(P小于10(-6))。累计而言,在S-180小鼠中,460个位点中有50个(10.9%)感染了易位的GI细菌,而对照动物中485个位点中只有9个(1.9%)(P小于10(-7))。胃肠道细菌通常易位,可以感染荷瘤小鼠的多个部位,但不能感染对照组。有氧革兰氏阴性杆菌在荷瘤小鼠中易位11次,但在对照组中仅易位1次,即使这些细菌的盲肠盲肠种群平均水平相对较低(范围为每g 4.33至5.28 log10个细菌)。在整个观察期间,S-180和对照小鼠的盲肠需氧细菌的种群水平相似。当S-180注射后4或8天致敏时,S-180小鼠具有显着抑制(P小于0.04)的迟发型超敏反应和血清血凝素反应。 S-180的生长与嗜中性白细胞增多和血小板计数略有下降有关。没有发现出血。因此,在免疫抑制的S-180小鼠中,革兰氏阴性杆菌和其他本地好氧细菌从胃肠道向肠系膜淋巴结及其他器官的转运增加,而这种增加并不是由肠道或细菌过度生长引起的。中性粒细胞减少症。

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