an ancient family of selb elongation factor-like proteins with a broad but disjunct distribution across archaea一个古老家族的selb伸长因子蛋白质广泛但古生菌的分离的分布.pdfVIP
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an ancient family of selb elongation factor-like proteins with a broad but disjunct distribution across archaea一个古老家族的selb伸长因子蛋白质广泛但古生菌的分离的分布
Atkinson et al. BMC Evolutionary Biology 2011, 11:22
/1471-2148/11/22
RESEARCH ARTICLE Open Access
An ancient family of SelB elongation factor-like
proteins with a broad but disjunct distribution
across archaea
*
Gemma C Atkinson , Vasili Hauryliuk, Tanel Tenson
Abstract
Background: SelB is the dedicated elongation factor for delivery of selenocysteinyl-tRNA to the ribosome. In
archaea, only a subset of methanogens utilizes selenocysteine and encodes archaeal SelB (aSelB). A SelB-like
(aSelBL) homolog has previously been identified in an archaeon that does not encode selenosysteine, and has
been proposed to be a pyrrolysyl-tRNA-specific elongation factor (EF-Pyl). However, elongation factor EF-Tu is
capable of binding archaeal Pyl-tRNA in bacteria, suggesting the archaeal ortholog EF1A may also be capable of
delivering Pyl-tRNA to the ribosome without the need of a specialized factor.
Results: We have phylogenetically characterized the aSelB and aSelBL families in archaea. We find the distribution
of aSelBL to be wider than both selenocysteine and pyrrolysine usage. The aSelBLs also lack the carboxy terminal
domain usually involved in recognition of the selenocysteine insertion sequence in the target mRNA. While most
aSelBL-encoding archaea are methanogenic Euryarchaea, we also find aSelBL representatives in Sulfolobales and
Thermoproteales of Crenarchaea, and in the recently identified phylum Thaumarchaea, suggesting that aSelBL
evolution has involved horizontal gene transfer and/or parallel loss. Severe disruption of the GTPase domain
suggests that some family members may employ a hitherto unknown mechanism of nucleotide hydrolysis, or have
lost their GTPase ability altogether. However, patterns of sequence conservation indicate that aSelBL is still capable
of binding the ribosome and am
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