Cytochrome P450 structure anatomy – recognition and analysis of
secondary structure elements

MIDLIK, Adam, Radka SVOBODOVÁ VAŘEKOVÁ, Veronika NAVRÁTILOVÁ, Karel BERKA a Jaroslav KOČA. Cytochrome P450 structure anatomy – recognition and analysis of secondary structure elements. In ISMB/ECCB, Prague. 2017.

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TY  - CONF
ID  - 1608522
AU  - Midlik, Adam - Svobodová Vařeková, Radka - Navrátilová, Veronika - Berka, Karel - Koča, Jaroslav
PY  - 2017
TI  - Cytochrome P450 structure anatomy – recognition and analysis of secondary structure elements
UR  - https://www.iscb.org/ismbeccb2017
N2  - Nowadays, structural bioinformatics faces an enormous growth in the number of available protein structures. Moreover, structurally similar proteins form protein families and these families represent rich datasets. In order to understand their molecular function we must focus on the key structural regions (binding sites, channels, allosteric sites, etc.), which involve both conserved and variable regions. Number and position of secondary structure elements (helices and sheets) is usually highly conserved within each protein family, thus they can serve as a firm point for identification of these key regions. Cytochromes P450 are proteins responsible for degradation of drugs and other xenobiotic substances in the organism and thus understanding of their function is crucial in drug design. They are an example of a protein family where the secondary structure elements are traditionally annotated with fixed names, facilitating description and comparison of their structures in the literature. In the last few years, the number of resolved cytochrome P450 structures has grown markedly and currently there are available more than 700 structures originating from more than 50 different organisms. Conserved annotation motivated us to analyze secondary structure elements across the whole cytochrome P450 family. During this process, we first developed an algorithm for automated annotation of secondary structure elements based on a template protein annotation. Secondly, we described the general anatomy and variability of cytochromes P450, based on this annotation. Specifically, we report features of their secondary structure elements such as frequency of occurrence, typical length, amino acid composition, and relation to the source organism.
ER  -

Základní údaje
Originální název	Cytochrome P450 structure anatomy – recognition and analysis of secondary structure elements
Autoři	MIDLIK, Adam, Radka SVOBODOVÁ VAŘEKOVÁ, Veronika NAVRÁTILOVÁ, Karel BERKA a Jaroslav KOČA.
Vydání	ISMB/ECCB, Prague, 2017.

Další údaje
Originální jazyk	angličtina
Typ výsledku	Konferenční abstrakt
Obor	10608 Biochemistry and molecular biology
Stát vydavatele	Česká republika
Utajení	není předmětem státního či obchodního tajemství
WWW	URL
Organizační jednotka	Přírodovědecká fakulta
Příznaky	Mezinárodní význam
Změnil	Změnil: Mgr. et Mgr. Adam Midlik, Ph.D., učo 379962. Změněno: 22. 1. 2020 13:41.

Anotace

Nowadays, structural bioinformatics faces an enormous growth in the number of available protein structures. Moreover, structurally similar proteins form protein families and these families represent rich datasets. In order to understand their molecular function we must focus on the key structural regions (binding sites, channels, allosteric sites, etc.), which involve both conserved and variable regions. Number and position of secondary structure elements (helices and sheets) is usually highly conserved within each protein family, thus they can serve as a firm point for identification of these key regions. Cytochromes P450 are proteins responsible for degradation of drugs and other xenobiotic substances in the organism and thus understanding of their function is crucial in drug design. They are an example of a protein family where the secondary structure elements are traditionally annotated with fixed names, facilitating description and comparison of their structures in the literature. In the last few years, the number of resolved cytochrome P450 structures has grown markedly and currently there are available more than 700 structures originating from more than 50 different organisms. Conserved annotation motivated us to analyze secondary structure elements across the whole cytochrome P450 family. During this process, we first developed an algorithm for automated annotation of secondary structure elements based on a template protein annotation. Secondly, we described the general anatomy and variability of cytochromes P450, based on this annotation. Specifically, we report features of their secondary structure elements such as frequency of occurrence, typical length, amino acid composition, and relation to the source organism.

VytisknoutZobrazeno: 7. 5. 2024 16:12

Cytochrome P450 structure anatomy – recognition and analysis of secondary structure elements

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