FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4383818032> ?p ?o ?g. }

• W4383818032 endingPage "1532" @default.
• W4383818032 startingPage "1532" @default.
• W4383818032 abstract "AKT1 is a serine/threonine kinase necessary for the mediation of apoptosis, angiogenesis, metabolism, and cell proliferation in both normal and cancerous cells. The mutations in the AKT1 gene have been associated with different types of cancer. Further, the AKT1 gene mutations are also reported to be associated with other diseases such as Proteus syndrome and Cowden syndromes. Hence, this study aims to identify the deleterious AKT1 missense SNPs and predict their effect on the function and structure of the AKT1 protein using various computational tools.Extensive in silico approaches were applied to identify deleterious SNPs of the human AKT1 gene and assessment of their impact on the function and structure of the AKT1 protein. The association of these highly deleterious missense SNPs with different forms of cancers was also analyzed. The in silico approach can help in reducing the cost and time required to identify SNPs associated with diseases.In this study, 12 highly deleterious SNPs were identified which could affect the structure and function of the AKT1 protein. Out of the 12, four SNPs-namely, G157R, G159V, G336D, and H265Y-were predicted to be located at highly conserved residues. G157R could affect the ligand binding to the AKT1 protein. Another highly deleterious SNP, R273Q, was predicted to be associated with liver cancer.This study can be useful for pharmacogenomics, molecular diagnosis of diseases, and developing inhibitors of the AKT1 oncogene." @default.
• W4383818032 created "2023-07-11" @default.
• W4383818032 creator A5000116814 @default.
• W4383818032 creator A5006652253 @default.
• W4383818032 creator A5021125047 @default.
• W4383818032 creator A5037021649 @default.
• W4383818032 creator A5080855773 @default.
• W4383818032 date "2023-07-10" @default.
• W4383818032 modified "2023-09-26" @default.
• W4383818032 title "Discovering Deleterious Single Nucleotide Polymorphisms of Human AKT1 Oncogene: An In Silico Study" @default.
• W4383818032 cites W1563940013 @default.
• W4383818032 cites W1683278196 @default.
• W4383818032 cites W1735389905 @default.
• W4383818032 cites W1774774834 @default.
• W4383818032 cites W1899479364 @default.
• W4383818032 cites W1939472951 @default.
• W4383818032 cites W1981506621 @default.
• W4383818032 cites W1981711832 @default.
• W4383818032 cites W2001326517 @default.
• W4383818032 cites W2007114641 @default.
• W4383818032 cites W2007215370 @default.
• W4383818032 cites W2010190071 @default.
• W4383818032 cites W2018023891 @default.
• W4383818032 cites W2029025258 @default.
• W4383818032 cites W2037591877 @default.
• W4383818032 cites W2043482853 @default.
• W4383818032 cites W2049041885 @default.
• W4383818032 cites W2049363668 @default.
• W4383818032 cites W2058487877 @default.
• W4383818032 cites W2059145105 @default.
• W4383818032 cites W2065674479 @default.
• W4383818032 cites W2070643112 @default.
• W4383818032 cites W2074695992 @default.
• W4383818032 cites W2088140119 @default.
• W4383818032 cites W2089335658 @default.
• W4383818032 cites W2090004564 @default.
• W4383818032 cites W2090649877 @default.
• W4383818032 cites W2102245393 @default.
• W4383818032 cites W2103210604 @default.
• W4383818032 cites W2109372707 @default.
• W4383818032 cites W2111326065 @default.
• W4383818032 cites W2112480941 @default.
• W4383818032 cites W2121519777 @default.
• W4383818032 cites W2122133437 @default.
• W4383818032 cites W2131900949 @default.
• W4383818032 cites W2136513422 @default.
• W4383818032 cites W2137886330 @default.
• W4383818032 cites W2140538197 @default.
• W4383818032 cites W2147941657 @default.
• W4383818032 cites W2151460035 @default.
• W4383818032 cites W2167663587 @default.
• W4383818032 cites W2168621448 @default.
• W4383818032 cites W2169678694 @default.
• W4383818032 cites W2171464043 @default.
• W4383818032 cites W2300696561 @default.
• W4383818032 cites W2376573086 @default.
• W4383818032 cites W2397963384 @default.
• W4383818032 cites W2406780350 @default.
• W4383818032 cites W2604998164 @default.
• W4383818032 cites W2605565630 @default.
• W4383818032 cites W2606513998 @default.
• W4383818032 cites W2607129810 @default.
• W4383818032 cites W2609082695 @default.
• W4383818032 cites W2782733462 @default.
• W4383818032 cites W2791771217 @default.
• W4383818032 cites W2793259154 @default.
• W4383818032 cites W2896744886 @default.
• W4383818032 cites W2919705191 @default.
• W4383818032 cites W2955065634 @default.
• W4383818032 cites W2979047242 @default.
• W4383818032 cites W2992895139 @default.
• W4383818032 cites W3000332676 @default.
• W4383818032 cites W3007654924 @default.
• W4383818032 cites W3008545150 @default.
• W4383818032 cites W3011895364 @default.
• W4383818032 cites W3012344944 @default.
• W4383818032 cites W3017755479 @default.
• W4383818032 cites W3020440546 @default.
• W4383818032 cites W3082144258 @default.
• W4383818032 cites W3082475372 @default.
• W4383818032 cites W3106856019 @default.
• W4383818032 cites W3107527779 @default.
• W4383818032 cites W3118865711 @default.
• W4383818032 cites W3119682700 @default.
• W4383818032 cites W3128231101 @default.
• W4383818032 cites W3135111815 @default.
• W4383818032 cites W3168622161 @default.
• W4383818032 cites W4213459840 @default.
• W4383818032 cites W4281993476 @default.
• W4383818032 cites W4361807030 @default.
• W4383818032 doi "https://doi.org/10.3390/life13071532" @default.
• W4383818032 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/37511907" @default.
• W4383818032 hasPublicationYear "2023" @default.
• W4383818032 type Work @default.
• W4383818032 citedByCount "0" @default.
• W4383818032 crossrefType "journal-article" @default.
• W4383818032 hasAuthorship W4383818032A5000116814 @default.
• W4383818032 hasAuthorship W4383818032A5006652253 @default.

• next