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利用猴和转基因小鼠模型开发抗结核病的治疗性和预防性疫苗。

Development of therapeutic and prophylactic vaccine against Tuberculosis using monkey and transgenic mice models.

作者信息

Kita Yoko, Okada Masaji, Nakajima Toshihiro, Kanamaru Noriko, Hashimoto Satomi, Nagasawa Tetsuji, Kaneda Yasufumi, Yoshida Shigeto, Nishida Yasuko, Nakatani Hitoshi, Takao Kyoko, Kishigami Chie, Nishimatsu Shiho, Sekine Yuki, Takamori Yasushi, McMurray David N, De la Cruz E C, Tan E V, Abalos R M, Burgos J A, Saunderson Paul, Sakatani Mitsunori

机构信息

Clinical Research Center, National Hospital Organization Kinki-chuo Chest Medical Center, Kitaku, Sakai, Osaka, Japan.

出版信息

Hum Vaccin. 2011 Jan-Feb;7 Suppl:108-14. doi: 10.4161/hv.7.0.14571. Epub 2011 Jan 1.

Abstract

PURPOSE

BCG is not efficacious against M. tuberculosis (TB) in adult. Therefore, novel TB vaccines were established by using three kinds of animal models (cynomolgus monkey model which is the best animal model of human TB, IL-2R knock out SCID mice as a human immune model, and granulysin transgenic mouse).

METHODS AND RESULTS

DNA vaccine expressing TB Hsp65 and IL-12 was delivered by the hemagglutinating virus of Japan (HVJ)-envelope. The BCG prime followed by Hsp65+IL-12/HVJ vaccine boost showed a synergistic effect in the TB-infected cynomolgus monkey (100% survival). In contrast, 33% of monkeys were alive in BCG alone group. Furthermore, the prolongation of survival period of the monkey was observed by the combination of BCG and DNA vaccine even when the boost was performed after long-term period (4month) from prime. This combination also improved the erythrocyte sedimentation rate (ESR), increased the body weight, and augmented the proliferation of PBL and IL-12 production at higher levels than BCG alone or saline. Furthermore, this vaccine exerted therapeutic efficacy in IL-2R knock out SCID-PBL/hu mice, which were transplanted with human T cells. Granulysin is an important defensive molecule expressed by human T cells and NK cells and has a cytolytic activity against microbes including Mycobacterium tuberculosis (TB) and tumors. Expression of 15kD (15K) granulysin protein and mRNA in CD8 positive T cells in the patients infected with drug sensitive (TB) or multi-drug resistant (MDR-TB) M. tuberculosis were lower than that in the healthy volunteers, suggesting that granulysin treatment might improve the tuberculous disease in human. Therefore, we established two kinds of granulysin transgenic mice (15K granulysin transgenic mice and 9K granulysin transgenic mice). It was demonstrated that 15K granulysin transgenic mice as well as 9K granulysin transgenic mice exerted in vivo anti-TB effect, including the decrease of the number of TB and augmentation of the CTL activity. These are the first findings which demonstrate in vivo effects of 15K granulysin and 9K granulysin against TB infection. Moreover, DNA vaccine expressing 15K granulysin showed a therapeutic activity against TB in mice.

CONCLUSION

These data indicate that monkey, IL-2R gene-knock out SCID-PBL/hu and granulysin transgenic mice models provide useful tools for the development of novel vaccines (HVJ-Envelope/Hsp65 DNA + IL-12 DNA vaccine and granulysin vaccine) against TB.

摘要

目的

卡介苗对成人结核分枝杆菌(TB)无效。因此,利用三种动物模型(食蟹猴模型,其是人类结核病的最佳动物模型;IL-2R基因敲除的SCID小鼠作为人类免疫模型;颗粒溶素转基因小鼠)建立了新型结核病疫苗。

方法与结果

表达结核热休克蛋白65(Hsp65)和白细胞介素-12(IL-12)的DNA疫苗通过日本血凝病毒(HVJ)包膜递送。先用卡介苗初免,再用Hsp65+IL-12/HVJ疫苗加强免疫,在感染结核的食蟹猴中显示出协同效应(100%存活)。相比之下,单独使用卡介苗组33%的猴子存活。此外,即使在初免后很长一段时间(4个月)进行加强免疫,卡介苗与DNA疫苗联合使用也能观察到猴子存活期延长。这种联合还改善了红细胞沉降率(ESR),增加了体重,并且比单独使用卡介苗或生理盐水更显著地提高了外周血淋巴细胞(PBL)的增殖和IL-12的产生。此外,这种疫苗在移植了人类T细胞的IL-2R基因敲除的SCID-PBL/hu小鼠中发挥了治疗效果。颗粒溶素是人类T细胞和自然杀伤细胞表达的一种重要防御分子,对包括结核分枝杆菌(TB)和肿瘤在内的微生物具有细胞溶解活性。在感染药物敏感型(TB)或耐多药型(MDR-TB)结核分枝杆菌的患者中,CD8阳性T细胞中15kD(15K)颗粒溶素蛋白和mRNA的表达低于健康志愿者,这表明颗粒溶素治疗可能改善人类结核病。因此,我们建立了两种颗粒溶素转基因小鼠(15K颗粒溶素转基因小鼠和9K颗粒溶素转基因小鼠)。结果表明,15K颗粒溶素转基因小鼠和9K颗粒溶素转基因小鼠均具有体内抗结核作用,包括减少结核数量和增强细胞毒性T淋巴细胞(CTL)活性。这些是首次证明15K颗粒溶素和9K颗粒溶素对结核感染具有体内作用的研究结果。此外,表达15K颗粒溶素的DNA疫苗在小鼠中显示出抗结核治疗活性。

结论

这些数据表明,猴子、IL-2R基因敲除的SCID-PBL/hu小鼠和颗粒溶素转基因小鼠模型为开发抗结核新型疫苗(HVJ包膜/Hsp65 DNA+IL-12 DNA疫苗和颗粒溶素疫苗)提供了有用的工具。

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