首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Low zone tolerance to contact allergens in mice: a functional role for CD8+ T helper type 2 cells
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Low zone tolerance to contact allergens in mice: a functional role for CD8+ T helper type 2 cells

机译:小鼠接触过敏原的区域耐受力低:CD8 + T辅助细胞2型细胞的功能性作用

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摘要

Normal skin is permeable to low molecular hydrophobic substances, including allergenic chemicals. Whereas such foreign matter appears to enter the skin naturally, it rarely induces contact hypersensitivity. This suggests that immunological tolerance would be the normal state of affairs. In search of a suitable model, we painted picryl chloride or oxazolone once or repeatedly on normal skin of BALB/c or C57B1/6 mice and found subsensitizing doses to be tolerogenic. The most effective doses in inducing tolerance were doses between those at the point of inflection from no responses to threshold sensitivity. But even doses three orders of magnitude lower than these suppressed subsequent sensitization if applied repeatedly. C57B1/6 mice (low responders) were consistently easier to make tolerant than BALB/c mice (high responders). The tolerant state established by a single painting was found to be fully developed at 48 h after initiation and long-lasting (>14 d). It could be adoptively transferred by intravenous injection of total spleen cells (SC), lymph node cells (LNC), or purified T cells and shown to be hapten specific. Pretreatment with cyclophosphamide (Cy) prevented tolerization. The T cells capable of transferring suppressive activity were found to be generated irrespective of the dose applied. On day 2 after painting, tolerance could be transferred with LNC from both tolerant and sensitized animals. On day 5, however, only cells from tolerant donors transferred tolerance. But by action of Cy, suppression was shown to be part of every sensitization, although masked. Production of hapten-specific antibodies was suppressed as well. Through depletion by monoclonal antibody in vitro the T suppressor cells were shown to belong to the murine CD8+ subset (Lyt2+). Upon restimulation in vitro by haptenized and irradiated normal SC, LNC from tolerant donors produced predominantly interleukin (IL)-4, IL-5, and IL-10. In contrast, LNC from sensitized donors produced preferentially IL-2 and interferon-gamma. Thus we demonstrate that painting subsensitizing doses of contact sensitizers on normal murine skin generates CD8+ Th2-like cells that give rise to hapten- specific tolerance. The model may have broader significance and apply to other species, including humans.
机译:正常皮肤可渗透包括过敏原化学物质在内的低分子疏水性物质。尽管这些异物似乎自然地进入皮肤,但很少引起接触性超敏反应。这表明免疫耐受将是正常情况。为了寻找合适的模型,我们在BALB / c或C57B1 / 6小鼠的正常皮肤上一次或多次涂抹了氯化聚甲基吡啶或恶唑酮,并发现亚致敏剂量具有致耐受性。诱导耐受性的最有效剂量是在从无反应到阈值敏感性的拐点处的剂量。但是如果重复使用,即使比这些剂量低三个数量级的剂量也抑制了随后的致敏作用。 C57B1 / 6小鼠(低应答者)始终比BALB / c小鼠(高应答者)更容易耐受。发现由单幅画建立的耐受状态在引发和持续时间(> 14 d)后的48小时内已完全发展。可以通过静脉注射总脾细胞(SC),淋巴结细胞(LNC)或纯化的T细胞来过继转移,并证明是半抗原特异性的。用环磷酰胺(Cy)进行预处理可防止耐受性。发现不管施加的剂量如何,都能够产生能够转移抑制活性的T细胞。涂漆后的第2天,耐受性和致敏性动物均可通过LNC转移耐受性。然而,在第5天,仅来自耐受供体的细胞转移了耐受性。但是通过Cy的作用,抑制被显示为所有敏化的一部分,尽管被掩盖了。半抗原特异性抗体的产生也被抑制。通过体外单克隆抗体的耗竭,显示出T抑制细胞属于鼠CD8 +亚群(Lyt2 +)。经半抗原和辐射正常SC体外再刺激后,来自耐受性供体的LNC主要产生白介素(IL)-4,IL-5和IL-10。相反,来自致敏供体的LNC优先产生IL-2和干扰素-γ。因此,我们证明了在正常鼠科动物皮肤上绘画亚敏剂量的接触敏化剂会产生CD8 + Th2样细胞,从而引起半抗原特异性耐受。该模型可能具有更广泛的意义,并适用于其他物种,包括人类。

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