Ostreopsis cf.ovata is a marine benthic dinoflagellate in tropical and temperate seas and can produce potent toxic compounds.The existence of O.cf.ovata has been found in the Chinese coastal areas,but studies on its t...Ostreopsis cf.ovata is a marine benthic dinoflagellate in tropical and temperate seas and can produce potent toxic compounds.The existence of O.cf.ovata has been found in the Chinese coastal areas,but studies on its toxicity are very few.This study investigated the toxicity of the O.cf.ovata(TIO991)isolated from Weizhou Island in the South China Sea by using methanol and chloroform to extract toxic compounds from the algal cells cultured indoor.Experiments on mouse acute toxicity showed that the crude methanol extract(CME)of O.cf.ovata caused the death of mice in 16–18 min.Furthermore,CME inhibited the cell reproduction of human neuroblastoma cells(BE(2)-M17 cells)by Cell Counting Kit-8 with a dose-and time-effect relationship and caused cell death in the form of cell necrosis.We found that CME had strong hemolytic activity and was significantly inhibited by ouabain,indicating that CME might contain palytoxins.By contrast,the crude chloroform extract of O.cf.ovata was relatively weak in toxicity as obtained in our experiments on mouse acute toxicity,cytotoxicity,and hemolytic activity.This suggests that the algae may raise the potential threat to marine ecosystems and public health.展开更多
Human S100A7 (psoriasin) is highly expressed in psoriasis and other inflammatory diseases; however, the function of S100A7 in wound repair remains largely unknown. Here we demonstrated that skin injury increased the e...Human S100A7 (psoriasin) is highly expressed in psoriasis and other inflammatory diseases; however, the function of S100A7 in wound repair remains largely unknown. Here we demonstrated that skin injury increased the expression of S100A7. Damaged cells from wounded skin induced the expression of S100A7 via the activation of Toll-like receptor 3 (TLR3) followed by the activation of p38 MAPK. S100A7, in turn, acted on keratinocytes to induce the expression of terminal differentiation marker gene loricrin through the activation of p38 MAPK and caspase-1. The differentiation of keratinocytes induced by S100A7 resulted in skin stratification, thus efficiently promoting wound closure. Taken together, our results demonstrate that the activation of TLR3 accelerates wound closure via the induction of S100A7 to induce keratinocyte differentiation. These findings also provide new insights into the development of different forms of treatment with skin wounds.展开更多
基金Supported by the Special Research for the Science and Technology Basic Resources Investigation Program of China(No.2018FY100200)the National Natural Science Foundation of China(No.42176206)the Natural Science Foundation of Shandong Province(No.ZR2021MD071)。
文摘Ostreopsis cf.ovata is a marine benthic dinoflagellate in tropical and temperate seas and can produce potent toxic compounds.The existence of O.cf.ovata has been found in the Chinese coastal areas,but studies on its toxicity are very few.This study investigated the toxicity of the O.cf.ovata(TIO991)isolated from Weizhou Island in the South China Sea by using methanol and chloroform to extract toxic compounds from the algal cells cultured indoor.Experiments on mouse acute toxicity showed that the crude methanol extract(CME)of O.cf.ovata caused the death of mice in 16–18 min.Furthermore,CME inhibited the cell reproduction of human neuroblastoma cells(BE(2)-M17 cells)by Cell Counting Kit-8 with a dose-and time-effect relationship and caused cell death in the form of cell necrosis.We found that CME had strong hemolytic activity and was significantly inhibited by ouabain,indicating that CME might contain palytoxins.By contrast,the crude chloroform extract of O.cf.ovata was relatively weak in toxicity as obtained in our experiments on mouse acute toxicity,cytotoxicity,and hemolytic activity.This suggests that the algae may raise the potential threat to marine ecosystems and public health.
基金supported by the National Natural Science Foundation of China (31170867, 31470878, 31222021,81202327)the Science and Technology Commission of Shanghai Municipality (13JC1402301, 11DZ2260300)Shanghai Education Commission (13SG25), and Henry Fok Educational Foundation (141017)
文摘Human S100A7 (psoriasin) is highly expressed in psoriasis and other inflammatory diseases; however, the function of S100A7 in wound repair remains largely unknown. Here we demonstrated that skin injury increased the expression of S100A7. Damaged cells from wounded skin induced the expression of S100A7 via the activation of Toll-like receptor 3 (TLR3) followed by the activation of p38 MAPK. S100A7, in turn, acted on keratinocytes to induce the expression of terminal differentiation marker gene loricrin through the activation of p38 MAPK and caspase-1. The differentiation of keratinocytes induced by S100A7 resulted in skin stratification, thus efficiently promoting wound closure. Taken together, our results demonstrate that the activation of TLR3 accelerates wound closure via the induction of S100A7 to induce keratinocyte differentiation. These findings also provide new insights into the development of different forms of treatment with skin wounds.
