缺陷性Fas配体介导的细胞凋亡易导致肺支原体感染后慢性侵蚀性关节炎的发生。

Hsu H C, Zhang H G, Song G G, Xie J, Liu D, Yang P A, Fleck M, Wintersberger W, Zhou T, Edwards C K, Mountz J D

The University of Alabama at Birmingham, 35294-0007, USA.

Arthritis Rheum. 2001 Sep;44(9):2146-59. doi: 10.1002/1529-0131(200109)44:9<2146::AID-ART368>3.0.CO;2-O.

OBJECTIVE

To determine whether defective T cell apoptosis is associated with the development of a chronic arthritis subsequent to mycoplasma infection, and to determine whether deletion of T cells can prevent the development of this arthritis.

METHODS

B6 wild-type (B6-+/+), B6-lpr/lpr, and B6-gld/gld mice were infected with Mycoplasma pulmonis. The severity of lymphocytic infiltration and joint damage was evaluated, and the degree of recovery of viable mycoplasma from the spleen and joints was determined. Antigen-presenting cells derived from Fas mutant lpr mice (lpr-APC) were transfected ex vivo with an adenovirus (Ad) vector to yield lpr-APC expressing high levels of Fas ligand (lpr-APC-AdFasL), which in turn were transferred intraperitoneally into M pulmonis-infected B6-gld/gld mice. The development of arthritis subsequent to M pulmonis infection and the induction of apoptosis of cells within the synovial tissue and lymph nodes of lpr-APC-AdFasL-treated B6-gld/gld mice were determined.

RESULTS

Infection of B6-lpr/lpr and B6-gld/gld mice with M pulmonis resulted in an acute-phase inflammation of the synovium that later developed into a chronic erosive arthritis. Similar infection of B6-+/+ mice resulted only in an acute joint inflammatory response that resolved. Chronic arthritis in B6-gld/gld mice and B6-lpr/lpr was not due to persistent infection, since there were no differences in the rates of clearance of M pulmonis from the joints of B6-gld/gld or B6-lpr/lpr mice compared with B6-+/+ mice. Treatment of infected B6-gld/gld mice with lpr-APC-AdFasL resulted in a significantly decreased incidence of chronic arthritis that was associated with a decrease in lymph node T cells, but not with apoptosis of synovial T cells or fibroblasts.

CONCLUSION

Defective Fas/FasL-mediated apoptosis of T cells is an important factor that rendered arthritis-resistant B6 mice susceptible to the development of a chronic erosive arthritis subsequent to mycoplasma infection. In vivo lpr-APC-AdFasL cell-gene therapy is a safe and effective method for inhibiting the development of this arthritis.

目的

确定缺陷性T细胞凋亡是否与支原体感染后慢性关节炎的发生有关，以及确定T细胞的缺失能否预防这种关节炎的发生。

方法

用肺炎支原体感染B6野生型（B6-+/+）、B6-lpr/lpr和B6-gld/gld小鼠。评估淋巴细胞浸润和关节损伤的严重程度，并测定从脾脏和关节中回收的活支原体的程度。用腺病毒（Ad）载体对源自Fas突变lpr小鼠（lpr-APC）的抗原呈递细胞进行体外转染，以产生表达高水平Fas配体的lpr-APC（lpr-APC-AdFasL），然后将其腹腔内注射到感染肺炎支原体的B6-gld/gld小鼠体内。确定肺炎支原体感染后关节炎的发生情况以及lpr-APC-AdFasL处理的B6-gld/gld小鼠滑膜组织和淋巴结内细胞凋亡的诱导情况。

结果

用肺炎支原体感染B6-lpr/lpr和B6-gld/gld小鼠导致滑膜急性期炎症，随后发展为慢性侵蚀性关节炎。对B6-+/+小鼠进行类似感染仅导致急性关节炎症反应并消退。B6-gld/gld小鼠和B6-lpr/lpr小鼠的慢性关节炎并非由于持续感染，因为与B6-+/+小鼠相比，B6-gld/gld或B6-lpr/lpr小鼠关节中肺炎支原体的清除率没有差异。用lpr-APC-AdFasL治疗感染的B6-gld/gld小鼠导致慢性关节炎的发病率显著降低，这与淋巴结T细胞减少有关，但与滑膜T细胞或成纤维细胞凋亡无关。