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首页> 外文期刊>The Indian journal of medical research. >Studies of recombinant streptococcal pyrogenic exotoxin B/cysteine protease (rSPE B/SCP) in the skin of guinea pigs & the release of histamine from cultured mast cells & basophilic leukocytes.
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Studies of recombinant streptococcal pyrogenic exotoxin B/cysteine protease (rSPE B/SCP) in the skin of guinea pigs & the release of histamine from cultured mast cells & basophilic leukocytes.

机译:豚鼠皮肤重组链球菌热原性外毒素B /半胱氨酸蛋白酶(rSPE B / SCP)的研究以及培养的肥大细胞和嗜碱性白细胞中组胺的释放。

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摘要

BACKGROUND & OBJECTIVES: Streptococcal pyrogenic exotoxin B/streptococcal cysteine protease (SPE B/SCP) is considered to be one of the virulence factors of Streptococcus pyogenes (S. pyogenes) which causes serious diseases such as severe invasive infections and streptococcal toxic shock syndrome (STSS). There are no reports on the histamine releasing activity of SPE B/SCP from mast cells, although several biological activities have been studied. It is not clear whether SPE B/SCP have the superantigenic activity. We studied whether SPE B/SCP plays as a pathogenic factor in streptococcal infections and STSS through a histamine releasing activity. METHODS: Human mast cells and basophils were generated from CD34 positive cells isolated from cord blood and cultured in the presence of rIL-6, stem cell factor and/or rIL-3. The capacity of increasing capillary permeability of recombinant SPE B/SCP (rSPE B/SCP) was studied by using the skin of guinea pigs. Mitogenic activity to human T-cells of rSPE B/SCP was studied by incorporation of (3)Hthymidine. The levels of histamine in the plasma of patients with STSS and controls were measured by ELISA kit. RESULTS: rSPE B/SCP induced increased capillary permeability in the skin of guinea pigs, but both SPE A and SPE C did not exhibit such activity. Histamine was released from cultured human mast cells stimulated with rSPE B/SCP. The rSPE B/SCP did not exhibit mitogenic activity to human T-cells. Three of the 7 patients with STSS showed higher levels of plasma histamine than those of normal subjects. INTERPRETATION & CONCLUSION: The results suggested that increased capillary permeability and histamine release from mast cells induced by rSPE B/SCP might be involved in STSS and/or streptococcal infection of skin and mucous membrane.
机译:背景与目的:链球菌热原性外毒素B /链球菌半胱氨酸蛋白酶(SPE B / SCP)被认为是化脓性链球菌(S. pyogenes)的致病因子之一,可导致严重的疾病,例如严重的侵袭性感染和链球菌毒性休克综合征( STSS)。尽管已经研究了几种生物学活性,但没有关于肥大细胞中SPE B / SCP释放组胺活性的报道。 SPE B / SCP是否具有超抗原活性尚不清楚。我们研究了SPE B / SCP是否通过组胺释放活性作为链球菌感染和STSS的致病因素。方法:人肥大细胞和嗜碱性粒细胞是从脐带血分离的CD34阳性细胞中产生的,并在存在rIL-6,干细胞因子和/或rIL-3的情况下培养。利用豚鼠皮肤研究了重组SPE B / SCP(rSPE B / SCP)毛细血管通透性的提高能力。通过掺入(3)胸苷研究了rSPE B / SCP对人T细胞的致细胞分裂活性。用ELISA试剂盒测定STSS患者和对照组血浆中的组胺水平。结果:rSPE B / SCP诱导豚鼠皮肤毛细血管通透性增加,但SPE A和SPE C均未表现出这种活性。组胺从rSPE B / SCP刺激的培养的人类肥大细胞中释放。 rSPE B / SCP对人T细胞不显示有丝分裂活性。 7例STSS患者中有3例血浆组胺水平高于正常人。结论与结论:rSPE B / SCP诱导肥大细胞毛细血管通透性增加和组胺释放可能与皮肤粘膜STSS和/或链球菌感染有关。

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