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• W2998074414 endingPage "105684" @default.
• W2998074414 startingPage "105684" @default.
• W2998074414 abstract "During the growing process of the atherosclerotic lesions, lipid-filled macrophage foam cells form, accumulate, and ultimately undergo apoptotic death. If the apoptotic foam cells are not timely removed, they may undergo secondary necrosis, and form a necrotic lipid core which renders the plaque unstable and susceptible to rupture. Therefore, the non-lipid-filled fellow macrophages, as the main phagocytic cells in atherosclerotic lesions, need to effectively remove the apoptotic foam cells. In general, in apoptotic macrophages, caspases are the central regulators of several key processes required for their efficient efferocytosis. The processes include the generation of “Find-Me” signals (such as adenosine triphosphate/uridine triphosphate, fractalkine, lysophosphatidylcholine, and sphingosine-1-phosphate) for the recruitment of viable macrophages, generation of the Eat-Me signals (for example, phosphatidylserine) for the engulfment process, and, finally, release of anti-inflammatory mediators (including transforming factor β and interleukin-10) as a tolerance-enhancing and an anti-inflammatory response, and for the motile behavior of the apoptotic cell. The caspase-dependent mechanisms are operative also in apoptotic macrophages driving the atherogenesis. In this review, we explore the role of the molecular pathways related to the caspase-dependent events in efferocytosis in the context of atherosclerosis. Understanding of the molecular mechanisms of apoptotic cell death in atherosclerotic lesions is essential when searching for new leads to treat atherosclerosis." @default.
• W2998074414 created "2020-01-10" @default.
• W2998074414 creator A5033507359 @default.
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• W2998074414 creator A5053191492 @default.
• W2998074414 creator A5060135294 @default.
• W2998074414 creator A5085875890 @default.
• W2998074414 date "2020-03-01" @default.
• W2998074414 modified "2023-09-25" @default.
• W2998074414 title "Regulation of efferocytosis by caspase-dependent apoptotic cell death in atherosclerosis" @default.
• W2998074414 cites W1492302205 @default.
• W2998074414 cites W1532386517 @default.
• W2998074414 cites W1544269073 @default.
• W2998074414 cites W1845459216 @default.
• W2998074414 cites W1891826181 @default.
• W2998074414 cites W1940692702 @default.
• W2998074414 cites W1964064254 @default.
• W2998074414 cites W1965130745 @default.
• W2998074414 cites W1965270224 @default.
• W2998074414 cites W1968188734 @default.
• W2998074414 cites W1968789597 @default.
• W2998074414 cites W1969422685 @default.
• W2998074414 cites W1970388907 @default.
• W2998074414 cites W1971084572 @default.
• W2998074414 cites W1971530727 @default.
• W2998074414 cites W1975032025 @default.
• W2998074414 cites W1977449187 @default.
• W2998074414 cites W1999168822 @default.
• W2998074414 cites W2004035470 @default.
• W2998074414 cites W2004266769 @default.
• W2998074414 cites W2005861034 @default.
• W2998074414 cites W2008032729 @default.
• W2998074414 cites W2009789841 @default.
• W2998074414 cites W2010520310 @default.
• W2998074414 cites W2010835380 @default.
• W2998074414 cites W2021856025 @default.
• W2998074414 cites W2024299292 @default.
• W2998074414 cites W2025234694 @default.
• W2998074414 cites W2032758279 @default.
• W2998074414 cites W2033218668 @default.
• W2998074414 cites W2034643457 @default.
• W2998074414 cites W2035977785 @default.
• W2998074414 cites W2037141618 @default.
• W2998074414 cites W2040069166 @default.
• W2998074414 cites W2042851093 @default.
• W2998074414 cites W2044812837 @default.
• W2998074414 cites W2046150340 @default.
• W2998074414 cites W2046416443 @default.
• W2998074414 cites W2047641691 @default.
• W2998074414 cites W2049280533 @default.
• W2998074414 cites W2050449334 @default.
• W2998074414 cites W2056034929 @default.
• W2998074414 cites W2056123449 @default.
• W2998074414 cites W2057330104 @default.
• W2998074414 cites W2058543057 @default.
• W2998074414 cites W2065949777 @default.
• W2998074414 cites W2066171290 @default.
• W2998074414 cites W2071140344 @default.
• W2998074414 cites W2072623580 @default.
• W2998074414 cites W2075318281 @default.
• W2998074414 cites W2076911449 @default.
• W2998074414 cites W2078297328 @default.
• W2998074414 cites W2078489088 @default.
• W2998074414 cites W2080232041 @default.
• W2998074414 cites W2081245863 @default.
• W2998074414 cites W2082078082 @default.
• W2998074414 cites W2082259697 @default.
• W2998074414 cites W2084609653 @default.
• W2998074414 cites W2084623259 @default.
• W2998074414 cites W2092577537 @default.
• W2998074414 cites W2093212994 @default.
• W2998074414 cites W2095392779 @default.
• W2998074414 cites W2099076813 @default.
• W2998074414 cites W2099133435 @default.
• W2998074414 cites W2106361531 @default.
• W2998074414 cites W2106968981 @default.
• W2998074414 cites W2111300657 @default.
• W2998074414 cites W2113785203 @default.
• W2998074414 cites W2115457290 @default.
• W2998074414 cites W2117655042 @default.
• W2998074414 cites W2122693935 @default.
• W2998074414 cites W2126374403 @default.
• W2998074414 cites W2127514713 @default.
• W2998074414 cites W2127910234 @default.
• W2998074414 cites W2129723413 @default.
• W2998074414 cites W2138253156 @default.
• W2998074414 cites W2144779053 @default.
• W2998074414 cites W2146921697 @default.
• W2998074414 cites W2150642049 @default.
• W2998074414 cites W2152085321 @default.
• W2998074414 cites W2159330173 @default.
• W2998074414 cites W2161114503 @default.
• W2998074414 cites W2163254852 @default.
• W2998074414 cites W2163327518 @default.
• W2998074414 cites W2164159495 @default.
• W2998074414 cites W2204294107 @default.
• W2998074414 cites W2255264739 @default.

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