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W3163100588 endingPage "113535" @default.
W3163100588 startingPage "113535" @default.
W3163100588 abstract "Natural products and synthetic analogs have drawn much attention as potential therapeutical drugs to treat metabolic syndrome. We reviewed the underlying mechanisms of 32 natural products and analogs with potential pharmacological effects in vitro, and especially in rodent models and/or patients, that usually act on the PPAR pathway, along with other molecular targets. Recent outstanding total syntheses or semisyntheses of these lead compounds are stated. In general, they can activate the transcriptional activity of PPARα, PPARγ, PPARα/γ, PPARβ/δ, PPARα/δ, PPARγ/δ and panPPAR as weak, partial agonists or selective PPARγ modulators (SPPARγM), which may be useful for managing obesity, type 2 diabetes (T2D), dyslipidemia and non-fatty liver disease (NAFLD). Terpenoids is the largest group of compounds that act as potential modulators on PPARs and are comprised from small lipophilic cannabinoids to lipophilic pentacyclic triterpenes and polar saponins. Shikimates-phenylpropanoids include polar heterocyclic flavonoids and phenolic compounds containing at least one C3–C6 unit and usually a double bond on the propyl chain. Quercetin (19), resveratrol (24) and curcumin (27), stand out from this group for exhibiting beneficial effects on patients. Alkaloids, the minor group of potential modulators on PPARs, include berberine (30), which has been widely explored in preclinical and clinical studies for its potential beneficial effects on T2D and dyslipidemia. However, large-scale clinical trials may be warranted for the promising compounds." @default.
W3163100588 created "2021-05-24" @default.
W3163100588 creator A5009542582 @default.
W3163100588 creator A5012610428 @default.
W3163100588 creator A5027134593 @default.
W3163100588 creator A5056402238 @default.
W3163100588 creator A5078252901 @default.
W3163100588 date "2021-10-01" @default.
W3163100588 modified "2023-09-26" @default.
W3163100588 title "Natural products and analogs as preventive agents for metabolic syndrome via peroxisome proliferator-activated receptors: An overview" @default.
W3163100588 cites W1278892654 @default.
W3163100588 cites W1509405108 @default.
W3163100588 cites W1603379351 @default.
W3163100588 cites W1718233288 @default.
W3163100588 cites W1756692753 @default.
W3163100588 cites W1946314517 @default.
W3163100588 cites W1964189360 @default.
W3163100588 cites W1965647226 @default.
W3163100588 cites W1966991126 @default.
W3163100588 cites W1969013464 @default.
W3163100588 cites W1969209081 @default.
W3163100588 cites W1969356201 @default.
W3163100588 cites W1969395627 @default.
W3163100588 cites W1970439560 @default.
W3163100588 cites W1970509678 @default.
W3163100588 cites W1972123715 @default.
W3163100588 cites W1972659108 @default.
W3163100588 cites W1975120418 @default.
W3163100588 cites W1977041568 @default.
W3163100588 cites W1978425022 @default.
W3163100588 cites W1980237439 @default.
W3163100588 cites W1981963822 @default.
W3163100588 cites W1982621565 @default.
W3163100588 cites W1982926270 @default.
W3163100588 cites W1983400860 @default.
W3163100588 cites W1984883454 @default.
W3163100588 cites W1991932125 @default.
W3163100588 cites W1999278785 @default.
W3163100588 cites W2003504981 @default.
W3163100588 cites W2004140590 @default.
W3163100588 cites W2009263278 @default.
W3163100588 cites W2014742651 @default.
W3163100588 cites W2016593134 @default.
W3163100588 cites W2023354243 @default.
W3163100588 cites W2024299353 @default.
W3163100588 cites W2026088200 @default.
W3163100588 cites W2028797781 @default.
W3163100588 cites W2029321187 @default.
W3163100588 cites W2032612125 @default.
W3163100588 cites W2034134526 @default.
W3163100588 cites W2034310187 @default.
W3163100588 cites W2038286187 @default.
W3163100588 cites W2046208657 @default.
W3163100588 cites W2049746343 @default.
W3163100588 cites W2051886073 @default.
W3163100588 cites W2051990086 @default.
W3163100588 cites W2059202653 @default.
W3163100588 cites W2061840955 @default.
W3163100588 cites W2062116874 @default.
W3163100588 cites W2067942093 @default.
W3163100588 cites W2068398835 @default.
W3163100588 cites W2068500097 @default.
W3163100588 cites W2068973813 @default.
W3163100588 cites W2069933276 @default.
W3163100588 cites W2071063360 @default.
W3163100588 cites W2072362233 @default.
W3163100588 cites W2073365457 @default.
W3163100588 cites W2073578030 @default.
W3163100588 cites W2075199222 @default.
W3163100588 cites W2076432521 @default.
W3163100588 cites W2076553098 @default.
W3163100588 cites W2082466757 @default.
W3163100588 cites W2083319939 @default.
W3163100588 cites W2084062672 @default.
W3163100588 cites W2084802447 @default.
W3163100588 cites W2085901282 @default.
W3163100588 cites W2086505785 @default.
W3163100588 cites W2086713094 @default.
W3163100588 cites W2087613795 @default.
W3163100588 cites W2088583648 @default.
W3163100588 cites W2089354656 @default.
W3163100588 cites W2091479104 @default.
W3163100588 cites W2096478712 @default.
W3163100588 cites W2101964276 @default.
W3163100588 cites W2104904467 @default.
W3163100588 cites W2105316032 @default.
W3163100588 cites W2108169104 @default.
W3163100588 cites W2108534106 @default.
W3163100588 cites W2111217151 @default.
W3163100588 cites W2117680364 @default.
W3163100588 cites W2127178720 @default.
W3163100588 cites W2128211963 @default.
W3163100588 cites W2129205142 @default.
W3163100588 cites W2135009079 @default.
W3163100588 cites W2135167869 @default.
W3163100588 cites W2141314779 @default.
W3163100588 cites W2143104968 @default.
W3163100588 cites W2144590229 @default.