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首页> 外文期刊>Protein Engineering >TWO AMINO ACID MUTATIONS IN AN ANTI-HUMAN CD3 SINGLE CHAIN FV ANTIBODY FRAGMENT THAT AFFECT THE YIELD ON BACTERIAL SECRETION BUT NOT THE AFFINITY
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TWO AMINO ACID MUTATIONS IN AN ANTI-HUMAN CD3 SINGLE CHAIN FV ANTIBODY FRAGMENT THAT AFFECT THE YIELD ON BACTERIAL SECRETION BUT NOT THE AFFINITY

机译:抗人CD3单链FV抗体片段中的两种氨基酸突变,影响产量对细菌分泌的影响,但不影响亲和力

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摘要

Recombinant antibody fragments directed against cell surface antigens have facilitated the development of novel therapeutic agents. As a first step in the creation of cytotoxic immunoconjugates, we constructed a single-chain Fv fragment derived from the murine hybridoma OKT3, that recognizes an epitope on the epsilon-subunit of the human CD3 complex. Two amino acid residues were identified that are critical for the high level production of this scFv in Escherichia coil, First, the substitution of glutamic acid encoded by a PCR primer at position 6 of V-H framework 1 by glutamine led to a more than a 30-fold increase in the production of soluble scFv, Second, the substitution of cysteine by a serine in the middle of CDR-H3 additionally doubled the yield of soluble antibody fragment without any adverse effect on its affinity for the CD3 antigen, The double mutant scFv (Q,S) proved to be very stable in vitro: no loss of activity was observed after storage for 1 month at 4 degrees C, while the activity of scFv containing a cysteine residue in CDR-H3 decreased by more than half. The results of production yield, affinity, stability measurements and analysis of three-dimensional models of the structure suggest that the sixth amino acid influences the correct folding of the V-H domain, presumably by affecting a folding intermediate, but has no effect on antigen binding. [References: 52]
机译:针对细胞表面抗原的重组抗体片段促进了新型治疗剂的开发。作为创建细胞毒性免疫缀合物的第一步,我们构建了一种来自鼠类杂交瘤OKT3的单链Fv片段,该片段可识别人CD3复合物的ε-亚基上的表位。确定了两个氨基酸残基,这些残基对于在大肠杆菌中高水平生产此scFv至关重要。首先,由VH构架1的6位PCR引物编码的谷氨酸被谷氨酰胺取代,导致超过30-可溶性scFv产量增加三倍,其次,CDR-H3中间被丝氨酸取代的半胱氨酸使可溶性抗体片段的产量增加了一倍,而对CD3抗原的亲和力没有任何不利影响。 Q,S)被证明在体外非常稳定:在4℃下储存1个月后未观察到活性损失,而在CDR-H3中含有半胱氨酸残基的scFv的活性降低了一半以上。生产产量,亲和力,稳定性测量和结构三维模型的分析结果表明,第六种氨基酸可能会影响折叠中间物,从而影响V-H结构域的正确折叠,但对抗原结合没有影响。 [参考:52]

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