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• W2109757701 abstract "Pathologically elevated serum levels of fibroblast growth factor-23 (FGF23), a bone-derived hormone that regulates phosphorus homeostasis, result in renal phosphate wasting and lead to rickets or osteomalacia. Rarely, elevated serum FGF23 levels are found in association with mosaic cutaneous disorders that affect large proportions of the skin and appear in patterns corresponding to the migration of ectodermal progenitors. The cause and source of elevated serum FGF23 is unknown. In those conditions, such as epidermal and large congenital melanocytic nevi, skin lesions are variably associated with other abnormalities in the eye, brain and vasculature. The wide distribution of involved tissues and the appearance of multiple segmental skin and bone lesions suggest that these conditions result from early embryonic somatic mutations. We report five such cases with elevated serum FGF23 and bone lesions, four with large epidermal nevi and one with a giant congenital melanocytic nevus. Exome sequencing of blood and affected skin tissue identified somatic activating mutations of HRAS or NRAS in each case without recurrent secondary mutation, and we further found that the same mutation is present in dysplastic bone. Our finding of somatic activating RAS mutation in bone, the endogenous source of FGF23, provides the first evidence that elevated serum FGF23 levels, hypophosphatemia and osteomalacia are associated with pathologic Ras activation and may provide insight in the heretofore limited understanding of the regulation of FGF23." @default.
• W2109757701 created "2016-06-24" @default.
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• W2109757701 date "2013-09-04" @default.
• W2109757701 modified "2023-10-09" @default.
• W2109757701 title "Multilineage somatic activating mutations in HRAS and NRAS cause mosaic cutaneous and skeletal lesions, elevated FGF23 and hypophosphatemia" @default.
• W2109757701 cites W1494685702 @default.
• W2109757701 cites W1588987932 @default.
• W2109757701 cites W1826958270 @default.
• W2109757701 cites W1870235011 @default.
• W2109757701 cites W1965058394 @default.
• W2109757701 cites W1970305413 @default.
• W2109757701 cites W1971463078 @default.
• W2109757701 cites W1974807791 @default.
• W2109757701 cites W1975338079 @default.
• W2109757701 cites W1978253853 @default.
• W2109757701 cites W1979643551 @default.
• W2109757701 cites W1982130330 @default.
• W2109757701 cites W1982301490 @default.
• W2109757701 cites W1984515301 @default.
• W2109757701 cites W1984898235 @default.
• W2109757701 cites W1986409528 @default.
• W2109757701 cites W1990968874 @default.
• W2109757701 cites W1996729627 @default.
• W2109757701 cites W1999892434 @default.
• W2109757701 cites W2001279904 @default.
• W2109757701 cites W2002223230 @default.
• W2109757701 cites W2002494594 @default.
• W2109757701 cites W2004344897 @default.
• W2109757701 cites W2009773967 @default.
• W2109757701 cites W2011257826 @default.
• W2109757701 cites W2011349880 @default.
• W2109757701 cites W2012675371 @default.
• W2109757701 cites W2013973825 @default.
• W2109757701 cites W2014798701 @default.
• W2109757701 cites W2015319472 @default.
• W2109757701 cites W2020483173 @default.
• W2109757701 cites W2025424120 @default.
• W2109757701 cites W2028487693 @default.
• W2109757701 cites W2028782677 @default.
• W2109757701 cites W2032246226 @default.
• W2109757701 cites W2033746777 @default.
• W2109757701 cites W2035541415 @default.
• W2109757701 cites W2036676648 @default.
• W2109757701 cites W2040329227 @default.
• W2109757701 cites W2042200262 @default.
• W2109757701 cites W2043780110 @default.
• W2109757701 cites W2051959338 @default.
• W2109757701 cites W2057159445 @default.
• W2109757701 cites W2060635441 @default.
• W2109757701 cites W2062552972 @default.
• W2109757701 cites W2068226571 @default.
• W2109757701 cites W2070063902 @default.
• W2109757701 cites W2070397147 @default.
• W2109757701 cites W2070865790 @default.
• W2109757701 cites W2073706920 @default.
• W2109757701 cites W2075379726 @default.
• W2109757701 cites W2075788775 @default.
• W2109757701 cites W2080093621 @default.
• W2109757701 cites W2081546052 @default.
• W2109757701 cites W2083125043 @default.
• W2109757701 cites W2083237361 @default.
• W2109757701 cites W2086992071 @default.
• W2109757701 cites W2087189228 @default.
• W2109757701 cites W2088707626 @default.
• W2109757701 cites W2091765784 @default.
• W2109757701 cites W2094027090 @default.
• W2109757701 cites W2095112712 @default.
• W2109757701 cites W2099923692 @default.
• W2109757701 cites W2101903081 @default.
• W2109757701 cites W2101962120 @default.
• W2109757701 cites W2106701482 @default.
• W2109757701 cites W2108234281 @default.
• W2109757701 cites W2108469980 @default.
• W2109757701 cites W2109177164 @default.

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