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• W133024370 endingPage "26" @default.
• W133024370 startingPage "5" @default.
• W133024370 abstract "The analysis of genetic variation in candidate genes is an issue of central importance in pharmacogenomics. The specific approaches taken will have a critical impact on the successful identification of disease genes, the molecular correlates of drug response, and the establishment of meaningful relationships between genetic variants and phenotypes of biomedical and pharmaceutical importance in general. Against a historical background, this article distinguishes different approaches to candidate gene analysis, reflecting different stages in human genome research. Only recently has it become feasible to analyze genetic variation systematically at the ultimate level of resolution, ie, the DNA sequence. In this context, the importance of haplotype-based approaches to candidate gene analysis has at last been recognized; the determination of the specific combinations of variants for each of the two sequences of a gene defined as a haplotype is essential. An up-to-date summary of such maximum resolution data on the amount, nature, and structure of genetic variation in candidate genes will be given. These data demonstrate abundant gene sequence and haplotype diversity. Numerous individually different forms of a gene may exist. This presents major challenges to the analysis of relationships between genetic variation, gene function, and phenotype. First solutions seem within reach. The implications of naturally occurring variation for pharmacogenomics and personalized medicine are now evident. Future approaches to the identification, evaluation, and prioritization of drug targets, the optimization of clinical trials, and the development of efficient therapies must be based on in-depth knowledge of candidate gene variation as an essential prerequisite." @default.
• W133024370 created "2016-06-24" @default.
• W133024370 creator A5021256353 @default.
• W133024370 creator A5086522997 @default.
• W133024370 date "2004-03-31" @default.
• W133024370 modified "2023-09-26" @default.
• W133024370 title "Genetic variation and pharmacogenomics: concepts, facts, and challenges" @default.
• W133024370 cites W1502061430 @default.
• W133024370 cites W1506019467 @default.
• W133024370 cites W1508985588 @default.
• W133024370 cites W1511393905 @default.
• W133024370 cites W1528782506 @default.
• W133024370 cites W1533947687 @default.
• W133024370 cites W1543923901 @default.
• W133024370 cites W1583417996 @default.
• W133024370 cites W1583476286 @default.
• W133024370 cites W1603274157 @default.
• W133024370 cites W1604013791 @default.
• W133024370 cites W1628357539 @default.
• W133024370 cites W1642457845 @default.
• W133024370 cites W1670573097 @default.
• W133024370 cites W1711580613 @default.
• W133024370 cites W1965278426 @default.
• W133024370 cites W1965466890 @default.
• W133024370 cites W1966438086 @default.
• W133024370 cites W1969359572 @default.
• W133024370 cites W1974523504 @default.
• W133024370 cites W1984632007 @default.
• W133024370 cites W1992530497 @default.
• W133024370 cites W1994621921 @default.
• W133024370 cites W1995350947 @default.
• W133024370 cites W2001247487 @default.
• W133024370 cites W2008321551 @default.
• W133024370 cites W2012743573 @default.
• W133024370 cites W2013548837 @default.
• W133024370 cites W2018762866 @default.
• W133024370 cites W2022005040 @default.
• W133024370 cites W2022569130 @default.
• W133024370 cites W2022894439 @default.
• W133024370 cites W2025306791 @default.
• W133024370 cites W2028392560 @default.
• W133024370 cites W2030327143 @default.
• W133024370 cites W2035140293 @default.
• W133024370 cites W2042103448 @default.
• W133024370 cites W2043159401 @default.
• W133024370 cites W2044573154 @default.
• W133024370 cites W2045727226 @default.
• W133024370 cites W2047222949 @default.
• W133024370 cites W2048931131 @default.
• W133024370 cites W2060015298 @default.
• W133024370 cites W2061008984 @default.
• W133024370 cites W2062792922 @default.
• W133024370 cites W2062945269 @default.
• W133024370 cites W2062963521 @default.
• W133024370 cites W2063017492 @default.
• W133024370 cites W2064027072 @default.
• W133024370 cites W2064600045 @default.
• W133024370 cites W2071126398 @default.
• W133024370 cites W2072134379 @default.
• W133024370 cites W2073968357 @default.
• W133024370 cites W2074754379 @default.
• W133024370 cites W2076846196 @default.
• W133024370 cites W2079501979 @default.
• W133024370 cites W2089486914 @default.
• W133024370 cites W2098232388 @default.
• W133024370 cites W2099014586 @default.
• W133024370 cites W2105025553 @default.
• W133024370 cites W2105682384 @default.
• W133024370 cites W2106275464 @default.
• W133024370 cites W2110343195 @default.
• W133024370 cites W2116626047 @default.
• W133024370 cites W2121652923 @default.
• W133024370 cites W2122004833 @default.
• W133024370 cites W2123466824 @default.
• W133024370 cites W2127230663 @default.
• W133024370 cites W2127385343 @default.
• W133024370 cites W2128725994 @default.
• W133024370 cites W2129559300 @default.
• W133024370 cites W2133312667 @default.
• W133024370 cites W2134221074 @default.
• W133024370 cites W2135732313 @default.
• W133024370 cites W2137176025 @default.
• W133024370 cites W2145307001 @default.
• W133024370 cites W2149318232 @default.
• W133024370 cites W2152664025 @default.
• W133024370 cites W2154374078 @default.
• W133024370 cites W2157929834 @default.
• W133024370 cites W2159108856 @default.
• W133024370 cites W2160782760 @default.
• W133024370 cites W2161381121 @default.
• W133024370 cites W2168625835 @default.
• W133024370 cites W2168909179 @default.
• W133024370 cites W2169484904 @default.
• W133024370 cites W4254753097 @default.
• W133024370 cites W4294233345 @default.
• W133024370 cites W47147223 @default.
• W133024370 cites W93588716 @default.
• W133024370 doi "https://doi.org/10.31887/dcns.2004.6.1/mhoehe" @default.

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