Abstract:ObjectiveTo develop a novel oral delivery system for interleukin12 (IL12) using genetically engineered Bifidobacterium longum(B. longum) as the carrier and further evaluate the efficacy of IL12expressed B. longum on the coxsackievirus B3 (CVB3)induced myocarditis in mice.MethodsA mIL12 gene expression vector pBBADsIL12 for B. longum was constructed and transformed into Bifidobacterium, the expression of mIL12 in the engineered B. longum was identified in vitro by Western Blot and enzymelinked immunosorbent assay (ELISA) after Larabinose induction. BLAB/c mice were inoculated i.p. with infectious dose of CVB3 for fourteen days and were divided randomly into three groups. The IL12 group and green fluorescent protein group (GFP group) were orally administered with pBBADsIL12 and pBBADsGFP transformed B. longum for fourteen days respectively after the inoculation of the virus; saline group was administered i.p. with sterile PBS. All animals were killed in day 14 of treatment, and the murine hearts were dissected aseptically for hematoxylineosin (HE) staining, viral titer and RNA extraction for Th1 cell cytokines quantification.ResultsAfter 14 days of treatment, HE staining revealed that the severity of virusinduced myocarditis in IL12 group was reduced compared with that of GFP group and saline group; the percentage of cardiac pathological lesions and CVB3 titers in IL12 group was (18±5)% and (2.89±0.10)pfu/g respectively,which was significantly lower than that of GFP group ([31±6]%, [4.83±0.14]pfu/g) and saline group ([32±9]%, [4.80±0.15]pfu/g), respectively (all P<0.01); levels of interferonγ(IFNγ) and tumor necrosis factorα(TNFα) in cardiac tissue and supernatants of IL12 group was(2.27±0.15)pg/mL and (3.05±0.17)pg/mL, respectively, which was significantly higher than that of GFP group ([1.32±0.11]pg/mL,[2.37±0.16]pg/mL) and saline group ([1.38±0.11]pg/mL, [2.37±0.12]pg/mL), respectively (all P<0.01).ConclusionA novel oral delivery system of Bifidobacterium for murine IL12 has been successfully established. Oral administration of mIL12transformed B. longum may play a therapeutic role in the treatment of CVB3induced myocarditis in the mice.