Abstract
The deposition of Schistosoma japonicum (S. japonicum) eggs commonly induces inflammation, fibrosis, hyperplasia, ulceration, and polyposis in the colon, which poses a serious threat to human health. However, the underlying mechanism is largely neglected. Recently, the disorder of glucose and lipid metabolism was reported to participate in the liver fibrosis induced by the parasite, which provides a novel clue for studying the underlying mechanism of the intestinal pathology of the disease. This study focused on the metabolic reprogramming profiles of glucose and lipid in the colon of mice infected by S. japonicum. We found that S. japonicum infection shortened the colonic length, impaired intestinal integrity, induced egg-granuloma formation, and increased colonic inflammation. The expression of key enzymes involved in the pathways regulating glucose and lipid metabolism was upregulated in the colon of infected mice. Conversely, phosphatase and tensin homolog deleted on chromosome ten (PTEN) and its downstream signaling targets were significantly inhibited after infection. In line with these results, in vitro stimulation with soluble egg antigens (SEA) downregulated the expression of PTEN in CT-26 cells and induced metabolic alterations similar to that observed under in vivo results. Moreover, PTEN over-expression prevented the reprogramming of glucose and lipid metabolism induced by SEA in CT-26 cells. Overall, the present study showed that S. japonicum infection induces the reprogramming of glucose and lipid metabolism in the colon of mice, and PTEN may play a vital role in mediating this metabolic reprogramming. These findings provide a novel insight into the pathogenicity of S. japonicum in hosts.
Highlights
Schistosomiasis, a global neglected tropical disease (NTDS) caused by the organisms belonging to the genus Schistosoma, including S. japonicum, S. mansoni, and S. haematobium, is considered the second-most socially and economically devastating parasitic disease [1]
We found that S. japonicum infection induced the reprogramming of glucose and lipid metabolism in the intestine of mice, which accompanied with the inactivation of PTEN pathway
We observed that S. japonicum infection increased the mRNA levels of proinflammatory cytokines TNF-α, IL-6, IL-1β, and Monocyte chemotactic protein-1 (MCP-1) along with anti-inflammatory cytokines Transforming growth factor-β (TGF-β) and IL-10 in the colon
Summary
Schistosomiasis, a global neglected tropical disease (NTDS) caused by the organisms belonging to the genus Schistosoma, including S. japonicum, S. mansoni, and S. haematobium, is considered the second-most socially and economically devastating parasitic disease [1]. Polarized T-helper 2 (Th2)mediated immune responses are responsible for the development of chronic intestinal pathologies induced by schistosome eggs and soluble egg antigens (SEA) [6]. Many cell types, such as basophils, B cells, regulatory T cells (Treg), and dendritic cells (DCs), have been implicated in the induction or maintenance of Th2 responses against eggs and SEA [7,8,9]. Some independent studies in humans and rodents have demonstrated that fecal microbiome differences linked to host immuneregulation or inflammation are associated with parasitic infection [5, 10, 11]
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