FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2016185755> ?p ?o ?g. }

• W2016185755 endingPage "e1002118" @default.
• W2016185755 startingPage "e1002118" @default.
• W2016185755 abstract "Lengthy co-evolution of Homo sapiens and Mycobacterium tuberculosis, the main causative agent of tuberculosis, resulted in a dramatically successful pathogen species that presents considerable challenge for modern medicine. The continuous and ever increasing appearance of multi-drug resistant mycobacteria necessitates the identification of novel drug targets and drugs with new mechanisms of action. However, further insights are needed to establish automated protocols for target selection based on the available complete genome sequences. In the present study, we perform complete proteome level comparisons between M. tuberculosis, mycobacteria, other prokaryotes and available eukaryotes based on protein domains, local sequence similarities and protein disorder. We show that the enrichment of certain domains in the genome can indicate an important function specific to M. tuberculosis. We identified two families, termed pkn and PE/PPE that stand out in this respect. The common property of these two protein families is a complex domain organization that combines species-specific regions, commonly occurring domains and disordered segments. Besides highlighting promising novel drug target candidates in M. tuberculosis, the presented analysis can also be viewed as a general protocol to identify proteins involved in species-specific functions in a given organism. We conclude that target selection protocols should be extended to include proteins with complex domain architectures instead of focusing on sequentially unique and essential proteins only." @default.
• W2016185755 created "2016-06-24" @default.
• W2016185755 creator A5008774671 @default.
• W2016185755 creator A5028237788 @default.
• W2016185755 creator A5053727563 @default.
• W2016185755 creator A5073086096 @default.
• W2016185755 creator A5078144452 @default.
• W2016185755 date "2011-07-21" @default.
• W2016185755 modified "2023-10-17" @default.
• W2016185755 title "Proteins with Complex Architecture as Potential Targets for Drug Design: A Case Study of Mycobacterium tuberculosis" @default.
• W2016185755 cites W1551684330 @default.
• W2016185755 cites W1689761783 @default.
• W2016185755 cites W1906780201 @default.
• W2016185755 cites W1968698890 @default.
• W2016185755 cites W1978204846 @default.
• W2016185755 cites W1979076223 @default.
• W2016185755 cites W1982648171 @default.
• W2016185755 cites W1984393517 @default.
• W2016185755 cites W1984523365 @default.
• W2016185755 cites W1986250681 @default.
• W2016185755 cites W1988884004 @default.
• W2016185755 cites W1990650937 @default.
• W2016185755 cites W1992055692 @default.
• W2016185755 cites W1996038152 @default.
• W2016185755 cites W2000427888 @default.
• W2016185755 cites W2001097406 @default.
• W2016185755 cites W2006128966 @default.
• W2016185755 cites W2006192061 @default.
• W2016185755 cites W2009010596 @default.
• W2016185755 cites W2009455776 @default.
• W2016185755 cites W2011185704 @default.
• W2016185755 cites W2019249774 @default.
• W2016185755 cites W2020764576 @default.
• W2016185755 cites W2021563552 @default.
• W2016185755 cites W2022012591 @default.
• W2016185755 cites W2022110032 @default.
• W2016185755 cites W2022307447 @default.
• W2016185755 cites W2022659284 @default.
• W2016185755 cites W2028024933 @default.
• W2016185755 cites W2028415754 @default.
• W2016185755 cites W2039345443 @default.
• W2016185755 cites W2043519753 @default.
• W2016185755 cites W2044830639 @default.
• W2016185755 cites W2049476357 @default.
• W2016185755 cites W2049631853 @default.
• W2016185755 cites W2052606462 @default.
• W2016185755 cites W2055644676 @default.
• W2016185755 cites W2056169996 @default.
• W2016185755 cites W2058034454 @default.
• W2016185755 cites W2058558815 @default.
• W2016185755 cites W2059907843 @default.
• W2016185755 cites W2062409682 @default.
• W2016185755 cites W2063780770 @default.
• W2016185755 cites W2070496155 @default.
• W2016185755 cites W2075929473 @default.
• W2016185755 cites W2084652316 @default.
• W2016185755 cites W2085200152 @default.
• W2016185755 cites W2086987219 @default.
• W2016185755 cites W2091300474 @default.
• W2016185755 cites W2091586024 @default.
• W2016185755 cites W2091859563 @default.
• W2016185755 cites W2098732312 @default.
• W2016185755 cites W2099768941 @default.
• W2016185755 cites W2100380298 @default.
• W2016185755 cites W2100772783 @default.
• W2016185755 cites W2102267487 @default.
• W2016185755 cites W2106823660 @default.
• W2016185755 cites W2107190860 @default.
• W2016185755 cites W2112441403 @default.
• W2016185755 cites W2113985551 @default.
• W2016185755 cites W2120010485 @default.
• W2016185755 cites W2120744225 @default.
• W2016185755 cites W2121277457 @default.
• W2016185755 cites W2123634400 @default.
• W2016185755 cites W2125112523 @default.
• W2016185755 cites W2125604179 @default.
• W2016185755 cites W2127041573 @default.
• W2016185755 cites W2130395921 @default.
• W2016185755 cites W2131186249 @default.
• W2016185755 cites W2132521111 @default.
• W2016185755 cites W2135984873 @default.
• W2016185755 cites W2138778824 @default.
• W2016185755 cites W2139141437 @default.
• W2016185755 cites W2140354550 @default.
• W2016185755 cites W2142380475 @default.
• W2016185755 cites W2143061508 @default.
• W2016185755 cites W2148148140 @default.
• W2016185755 cites W2149472608 @default.
• W2016185755 cites W2153187042 @default.
• W2016185755 cites W2153971450 @default.
• W2016185755 cites W2156407548 @default.
• W2016185755 cites W2158023121 @default.
• W2016185755 cites W2158714788 @default.
• W2016185755 cites W2160517898 @default.
• W2016185755 cites W2161199282 @default.
• W2016185755 cites W2161303529 @default.
• W2016185755 cites W2164718888 @default.
• W2016185755 cites W2414307244 @default.

• next