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W4310248809 endingPage "14744" @default.
W4310248809 startingPage "14744" @default.
W4310248809 abstract "Inherited metabolic disorders (IMD) are rare medical conditions caused by genetic defects that interfere with the body’s metabolism. The clinical phenotype is highly variable and can present at any age, although it more often manifests in childhood. The number of treatable IMDs has increased in recent years, making early diagnosis and a better understanding of the natural history of the disease more important than ever. In this review, we discuss the main challenges faced in applying proteomics to the study of IMDs, and the key advances achieved in this field using tandem mass spectrometry (MS/MS). This technology enables the analysis of large numbers of proteins in different body fluids (serum, plasma, urine, saliva, tears) with a single analysis of each sample, and can even be applied to dried samples. MS/MS has thus emerged as the tool of choice for proteome characterization and has provided new insights into many diseases and biological systems. In the last 10 years, sequential window acquisition of all theoretical fragmentation spectra mass spectrometry (SWATH-MS) has emerged as an accurate, high-resolution technique for the identification and quantification of proteins differentially expressed between healthy controls and IMD patients. Proteomics is a particularly promising approach to help obtain more information on rare genetic diseases, including identification of biomarkers to aid early diagnosis and better understanding of the underlying pathophysiology to guide the development of new therapies. Here, we summarize new and emerging proteomic technologies and discuss current uses and limitations of this approach to identify and quantify proteins. Moreover, we describe the use of proteomics to identify the mechanisms regulating complex IMD phenotypes; an area of research essential to better understand these rare disorders and many other human diseases." @default.
W4310248809 created "2022-11-30" @default.
W4310248809 creator A5016682487 @default.
W4310248809 creator A5038022963 @default.
W4310248809 creator A5046954813 @default.
W4310248809 creator A5066412218 @default.
W4310248809 creator A5074969146 @default.
W4310248809 date "2022-11-25" @default.
W4310248809 modified "2023-10-05" @default.
W4310248809 title "Proteomics in Inherited Metabolic Disorders" @default.
W4310248809 cites W1120568487 @default.
W4310248809 cites W1498531581 @default.
W4310248809 cites W1561715092 @default.
W4310248809 cites W1836273607 @default.
W4310248809 cites W2004536300 @default.
W4310248809 cites W2010644723 @default.
W4310248809 cites W2013298107 @default.
W4310248809 cites W2017773668 @default.
W4310248809 cites W2019427729 @default.
W4310248809 cites W2039921716 @default.
W4310248809 cites W2052466566 @default.
W4310248809 cites W2075476568 @default.
W4310248809 cites W2076265228 @default.
W4310248809 cites W2077524059 @default.
W4310248809 cites W2077890471 @default.
W4310248809 cites W2079843936 @default.
W4310248809 cites W2081842591 @default.
W4310248809 cites W2099065449 @default.
W4310248809 cites W2129388952 @default.
W4310248809 cites W2134843051 @default.
W4310248809 cites W2146314061 @default.
W4310248809 cites W2153766856 @default.
W4310248809 cites W2153926022 @default.
W4310248809 cites W2172588665 @default.
W4310248809 cites W2188730791 @default.
W4310248809 cites W2323795628 @default.
W4310248809 cites W2338592504 @default.
W4310248809 cites W2403271797 @default.
W4310248809 cites W2524370798 @default.
W4310248809 cites W2533894695 @default.
W4310248809 cites W2587473769 @default.
W4310248809 cites W2593373303 @default.
W4310248809 cites W2604643952 @default.
W4310248809 cites W2605897603 @default.
W4310248809 cites W2759363431 @default.
W4310248809 cites W2771855438 @default.
W4310248809 cites W2789468179 @default.
W4310248809 cites W2807049387 @default.
W4310248809 cites W2887294942 @default.
W4310248809 cites W2889888677 @default.
W4310248809 cites W2891398396 @default.
W4310248809 cites W2893031871 @default.
W4310248809 cites W2896169521 @default.
W4310248809 cites W2903299964 @default.
W4310248809 cites W2905371653 @default.
W4310248809 cites W2905558973 @default.
W4310248809 cites W2909122637 @default.
W4310248809 cites W2915041558 @default.
W4310248809 cites W2934596651 @default.
W4310248809 cites W2944846836 @default.
W4310248809 cites W2947548522 @default.
W4310248809 cites W2947796929 @default.
W4310248809 cites W2948477377 @default.
W4310248809 cites W2972924932 @default.
W4310248809 cites W2974712087 @default.
W4310248809 cites W2979935292 @default.
W4310248809 cites W2980652521 @default.
W4310248809 cites W2988339276 @default.
W4310248809 cites W2995867266 @default.
W4310248809 cites W2997779568 @default.
W4310248809 cites W2998503646 @default.
W4310248809 cites W3006781731 @default.
W4310248809 cites W3021283721 @default.
W4310248809 cites W3025770323 @default.
W4310248809 cites W3026934493 @default.
W4310248809 cites W3037668580 @default.
W4310248809 cites W3039939852 @default.
W4310248809 cites W3092772923 @default.
W4310248809 cites W3094108931 @default.
W4310248809 cites W3096894426 @default.
W4310248809 cites W3102550459 @default.
W4310248809 cites W3113498109 @default.
W4310248809 cites W3117367755 @default.
W4310248809 cites W3134904637 @default.
W4310248809 cites W3135681293 @default.
W4310248809 cites W3139601120 @default.
W4310248809 cites W3155174346 @default.
W4310248809 cites W3172053221 @default.
W4310248809 cites W3173875945 @default.
W4310248809 cites W3193364683 @default.
W4310248809 cites W3201616316 @default.
W4310248809 cites W3209856620 @default.
W4310248809 cites W3215151924 @default.
W4310248809 cites W3216249353 @default.
W4310248809 cites W4214613209 @default.
W4310248809 cites W4220764901 @default.
W4310248809 cites W4220843472 @default.
W4310248809 cites W4224326364 @default.