首页> 美国卫生研究院文献>Biochemical Journal >Glutamine as a precursor to N-terminal pyrrolid-2-one-5-carboxylic acid in mouse immunoglobulin λ-type light chains. Amino acid-sequence variability at the N-terminal extra piece of λ-type light-chain precursors
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Glutamine as a precursor to N-terminal pyrrolid-2-one-5-carboxylic acid in mouse immunoglobulin λ-type light chains. Amino acid-sequence variability at the N-terminal extra piece of λ-type light-chain precursors

机译:谷氨酰胺作为小鼠免疫球蛋白λ型轻链中N末端吡咯烷-2-一-5-羧酸的前体。 λ型轻链前体N末端多余片段的氨基酸序列变异性

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摘要

The mRNA molecules coding for three mouse immunoglobulin λ-type light (L) chains (MOPC-104E λ1, RPC-20 λ1, MOPC-315 λ2) programme the cell-free synthesis of precursors larger than the mature proteins. Radioactive amino acid-sequence analyses of each of the three precursors labelled with [3H]alanine, [3H]serine, [3H]glutamine, [3H]glutamic acid and [3H]threonine showed that an extra piece, at least 18 residues long, is linked to the N-terminus of the mature L-chains. The N-terminal extra-peptide segment may be 19 residues long, since analyses of precursors labelled with [35S]methionine indicated an additional N-terminal methionine residue which was recovered in low yields. Presumably this is the initiator methionine, which is known to be short lived in eukaryotes. The mature forms of MOPC-104E, RPC-20 and MOPC-315 λ L-chains are blocked at the N-termini by pyrrolid-2-one-5-carboxylic acid (pyroglutamic acid). Sequence analyses of precursors labelled with [3H]glutamine and [3H]glutamic acid showed incorporation only of glutamine in a position that matches with the position of pyrrolid-2-one-5-carboxylic acid in the mature forms of all three precursors, and incorporation of glutamic acid in other positions. The data showed the absence of glutamine–glutamic acid interconversion, since the radioactive peaks obtained from either 3H-labelled amino acid were discrete, and free from cross-contamination. These results prove that glutamine is the precursor amino acid of pyrrolid-2-one-5-carboxylic acid at the N-termini of the mature MOPC-104E λ1, RPC-20 λ1 and MOPC-315 λ2 L-chains. Thus the formation of pyrrolid-2-one-5-carboxylic acid by cyclization of glutamine is a post-translational event which occurs after, or concomitant with, cleavage of the extra piece from the precursor to yield the mature L-chain. The variable (V) regions (110 amino acid residues) of mouse λ L-chains are quite similar: when compared with that of MOPC-104E λ1 chain, the V-region of RPC-20 λ1 chain differs in one residue, and the V-region of MOPC-315 λ2 chain differs in 11 residues. The partial sequence data show that the N-terminal extra pieces of the two λ1 L-chain precursors have, so far, identical partial sequences; the extra piece of the λ2 L-chain precursor differs from these in at least three out of 19 positions.
机译:编码三个小鼠免疫球蛋白λ型轻链(L)(MOPC-104Eλ1,RPC-20λ1,MOPC-315λ2)的mRNA分子可实现比成熟蛋白更大的前体的无细胞合成。 [ 3 H]丙氨酸,[ 3 H]丝氨酸,[ 3 H]标记的三种前体各自的放射性氨基酸序列分析]谷氨酰胺,[ 3 H]谷氨酸和[ 3 H]苏氨酸表明,至少有18个残基长的一个额外片段与谷氨酸的N末端连接。成熟的L链。 N末端肽段的长度可能为19个残基,因为对用[ 35 S]蛋氨酸标记的前体的分析表明,还有一个N末端蛋氨酸的残基可以低收率回收。据推测,这是引发剂蛋氨酸,它在真核生物中寿命短。 MOPC-104E,RPC-20和MOPC-315λL链的成熟形式在N末端被吡咯烷-2-一-5-羧酸(焦谷氨酸)封闭。用[ 3 H]谷氨酰胺和[ 3 H]谷氨酸标记的前体的序列分析表明,仅谷氨酰胺在与吡咯烷-2-位置匹配的位置掺入所有三种前体均以成熟形式存在1-5-羧酸,并在其他位置引入谷氨酸。数据表明不存在谷氨酰胺-谷氨酸的相互转化,因为从 3 H标记的氨基酸获得的放射性峰是离散的,并且没有交叉污染。这些结果证明,谷氨酰胺是在成熟的MOPC-104Eλ1,RPC-20λ1和MOPC-315λ2L链的N末端的吡咯烷-2-1-5-羧酸的前体氨基酸。因此,通过谷氨酰胺环化形成吡咯烷-2-一-5-羧酸是翻译后事件,其发生在多余片段从前体裂解以产生成熟的L链之后或与其同时发生。小鼠λL链的可变(V)区(110个氨基酸残基)非常相似:与MOPC-104Eλ1链相比,RPC-20λ1链的V区在一个残基上有所不同, MOPC-315λ2链的V区有11个残基。部分序列数据表明,到目前为止,两个λ1L链前体的N末端多余片段具有相同的部分序列;额外的λ2L链前体片段在19个位置中的至少三个位置与这些不同。

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