Greidinger Eric L, Zang YunJuan, Martinez Laisel, Jaimes Kimberly, Nassiri Mehdi, Bejarano Pablo, Barber Glen N, Hoffman Robert W
Veterans Affairs Medical Center, and the University of Miami Miller School of Medicine, Miami, Florida USA.
Arthritis Rheum. 2007 May;56(5):1589-97. doi: 10.1002/art.22601.
To assess the Y RNAs, a family of homologous RNAs that bind to the Ro autoantigen, for the ability to contribute to autoimmune disease by activating RNA-responsive Toll-like receptors (TLRs).
Using cell lines expressing or stably transfected with TLR-3, TLR-7, or TLR-8, we determined the patterns of RNA-specific TLR activation by in vitro transcripts of all of the known murine and human Y RNAs. Next, 8-10-week-old female mice were exposed to a single 50-microg subcutaneous injection of mouse Y1 or mouse Y3 RNA, and the effects were observed.
Y RNA family members differed in their TLR reactivities. Both human and mouse Y3 RNAs, but not other human or mouse Y RNAs, prominently induced TLR-3 activation. Although most human and mouse Y RNAs activated TLR-7 efficiently, mouse Y3 RNA and human Y5 RNA did not. Single subcutaneous injections of mice with either mouse Y1 RNA or mouse Y3 RNA induced or inhibited lymphoid infiltrates in different target organs based on the Y RNA and TLR status of the mouse used. Mouse Y1 RNA induced kidney lesions in TLR-3-intact mice but not in TLR-3-knockout mice. In contrast, mouse Y3 RNA treatment was associated with nephritis in TLR-3-knockout mice but not in TLR-3-intact mice. Sialoadenitis developed in untreated TLR-3-/- mice and in TLR-3-/- mice treated with mouse Y3 RNA, but sialoadenitis was not present in TLR--/-) mice treated with mouse Y1 RNA.
Y RNAs can induce innate immune responses and influence clinical manifestations of autoimmunity, suggesting that they are relevant to syndromes of anti-Ro autoimmunity. Distinct patterns of tissue targeting can be seen after exposure to different Y RNAs, in a pattern that correlates with the innate immune signals they induce. Thus, the balance of innate immune signals induced by exposure to endogenous Y RNAs may help determine the nature of the clinical syndrome in anti-Ro autoimmunity.
评估Y RNA(一类与Ro自身抗原结合的同源RNA)通过激活RNA反应性Toll样受体(TLR)促成自身免疫性疾病的能力。
利用表达或稳定转染TLR-3、TLR-7或TLR-8的细胞系,我们通过所有已知的小鼠和人类Y RNA的体外转录本确定了RNA特异性TLR激活模式。接下来,给8至10周龄的雌性小鼠皮下单次注射50微克小鼠Y1或小鼠Y3 RNA,并观察其效果。
Y RNA家族成员的TLR反应性不同。人类和小鼠的Y3 RNA均能显著诱导TLR-3激活,而其他人类或小鼠Y RNA则不能。尽管大多数人类和小鼠Y RNA能有效激活TLR-7,但小鼠Y3 RNA和人类Y5 RNA不能。根据所用小鼠的Y RNA和TLR状态,给小鼠单次皮下注射小鼠Y1 RNA或小鼠Y3 RNA会在不同靶器官诱导或抑制淋巴细胞浸润。小鼠Y1 RNA在TLR-3完整的小鼠中诱导肾脏病变,但在TLR-3基因敲除小鼠中则不会。相反,小鼠Y3 RNA处理与TLR-3基因敲除小鼠的肾炎相关,但在TLR-3完整的小鼠中则无此现象。未经处理的TLR-3 -/- 小鼠以及用小鼠Y3 RNA处理的TLR-3 -/- 小鼠会发生涎腺炎,但用小鼠Y1 RNA处理的TLR-3 -/- 小鼠则无涎腺炎。
Y RNA可诱导先天性免疫反应并影响自身免疫的临床表现,表明它们与抗Ro自身免疫综合征相关。接触不同Y RNA后可观察到不同的组织靶向模式,并与它们诱导的先天性免疫信号相关。因此,接触内源性Y RNA诱导的先天性免疫信号平衡可能有助于确定抗Ro自身免疫中临床综合征的性质。
