Polymerase I pathway inhibitor ameliorates experimental autoimmune encephalomyelitis
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- 作者:Anat Achiron ; Roi Mashiach ; Rina Zilkha-Falb ; Michael M. Meijler ; Michael Gurevich
- 关键词:Multiple sclerosis ; Experimental autoimmune encephalomyelitis ; Polymerase 1 pathway ; Polymerase 1 inhibitor ; Apoptosis
- 刊名:Journal of Neuroimmunology
- 出版年:2013
- 出版时间:15 October, 2013
- 年:2013
- 卷:263
- 期:1-2
- 页码:91-97
- 全文大小:1263 K
文摘
Applying high throughput gene expression microarrays we identified that the suppression of polymerase 1 (POL1) pathway is associated with benign course of multiple sclerosis (MS). This finding supports the rationale for direct targeting of the POL1 transcription machinery as an innovative strategy to suppress MS. To evaluate the effects of a specific polymerase I inhibitor (POL1-I) on experimental autoimmune encephalomyelitis (EAE), we immunized female C57BL/6J mice (8 weeks) with MOG35-55/CFA. A new POL1-I was administered at a daily dose of 12.5 mg/kg body weight by oral gavage either from the day of immunization until disease onset (EAE score 1.0, immunization model), at disease onset (EAE score = 1.0) for the following 14 days (treatment model), or by alternate daily dose of 25.0 mg/kg body weight, by oral gavage from the day of immunization for the following 25 days (combined model). POL1-I remarkably suppressed EAE in the immunization model; while in the Vehicle group the onset of EAE occurred on day 10.0 ¡À 0.4 with maximal clinical score of 3.2 ¡À 0.2, in the POL1-I treated mice onset was significantly delayed and occurred on day 16.9 ¡À 1.1 (p = 0.001), and maximal disease score 2.0 ¡À 0.1 was reduced (p = 0.004). In the treatment model POL1-I treatment significantly reduced disease activity; maximal score was 2.0 ¡À 0.5 while in the Vehicle group it reached a mean maximal score of 3.9 ¡À 0.1, (p = 0.0008). In the combined model, POL1-I treatment completely inhibited disease activity. The effect of POL1-I treatment was modulated through decreased expression of POL1 pathway key-related genes LRPPRC, pre-RNA, POLR1D and RRN3 together with activation of P53 dependent apoptosis of CD4 + splenocytes. Our findings demonstrate that POL1 pathway inhibition delayed and suppressed the development of EAE and ameliorated the disease in mice with persistent clinical signs.