首页> 美国卫生研究院文献>Journal of Virology >Asp-286----Asn-286 in polyomavirus large T antigen relaxes the specificity of binding to the polyomavirus origin.

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Asp-286----Asn-286 in polyomavirus large T antigen relaxes the specificity of binding to the polyomavirus origin.

机译：多瘤病毒中的大T抗原中的Asp-286 ---- Asn-286放松了与多瘤病毒源的结合特异性。

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摘要

We isolated revertants of a polyomavirus whose origin of DNA replication contains a point mutation in the palindrome to which large T antigen binds. Four independent second-site revertants contain an Asp-286----Asn-286 substitution in large T antigen. This mutant large T antigen activates replication of DNAs containing the mutant polyomavirus origin as well as replication of DNAs containing the wild-type origin; however, replication of DNAs with enhancer mutations is not activated by this large T antigen. The Asn-286 mutation occurs in a positively charge region of large T antigen near the location of several mutations which inactivate DNA replication. We suggest that this region of large T antigen is responsible for recognition of specific DNA sequences at the origin and that ionic forces are important for this interaction.

机译：我们分离了多瘤病毒的回复株，其DNA复制起点包含回文中与大T抗原结合的点突变。四个独立的第二位点回复子在大T抗原中包含Asp-286 ---- Asn-286取代。这种突变的大T抗原可激活含有突变多瘤病毒起源的DNA的复制以及含有野生型起源的DNA的复制。然而，具有增强子突变的DNA的复制并没有被这种大的T抗原激活。 Asn-286突变发生在大T抗原的带正电荷的区域中，靠近几个使DNA复制失活的突变的位置。我们建议大T抗原的此区域负责起源处特定DNA序列的识别，并且离子力对于这种相互作用很重要。

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期刊名称 Journal of Virology
作者
W J Tang; W R Folk;
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作者单位

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年(卷),期 1989(63),1
年度 1989
页码 242–249
总页数 8
原文格式 PDF
正文语种
中图分类人体病毒学（致病病毒）;病毒（滤过性病毒）;
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1. Characterization of highly frequent epitope-specific CD45RA+/CCR7+/- T lymphocyte responses against p53-binding domains of the human polyomavirus BK large tumor antigen in HLA-A*0201+ BKV-seropositive donors [J] . Maurizio Provenzano, Laura Bracci, Stephen Wyler, Journal of Translational Medicine . 2006,第1期

机译：表征针对HLA-A * 0201 + BKV血清反应阳性供体中人多瘤病毒BK大肿瘤抗原的p53结合域的频繁表位特异性CD45RA + / CCR7 +/- T淋巴细胞反应
2. DNA binding of polyomavirus large T‐antigen: kinetics of interactions with different types of binding sites [J] . Bondeson Karing, re, Magnusson Gouml, FEBS Letters . 1998,第3期

机译：多瘤病毒大T抗原的DNA结合：与不同类型结合位点相互作用的动力学
3. DNA binding of polyomavirus large T‐antigen: kinetics of interactions with different types of binding sites [J] . Bondeson Karing, re, Magnusson Gouml, FEBS Letters . 1998,第3期

机译：多瘤病毒大T抗原的DNA结合：与不同类型结合位点相互作用的动力学
4. STRUCTURES OF MERKEL CELL POLYOMAVIRUS VP1 COMPLEXES DEFINE A SIALIC ACID BINDING SITE REQUIRED FOR INFECTION [C] . Ursula Neu, Holger Hengel, Barbel S. Blaum International Carbohydrate Symposium . 2013

机译：Merkel Cell PolyomaVirus VP1复合物的结构定义了感染所需的唾液酸结合位点
5. Elucidating Mechanisms of Transformation and Tumorigenesis by Merkel Cell Polyomavirus Tumor Antigens [D] . Dye, Kristine Nicole. 2020

机译：Merkel CelloMavirus肿瘤抗原阐明转化和肿瘤发生机制
6. A short peptide eluted from the H-2Kb molecule of a polyomavirus-positive tumor corresponds to polyomavirus large T antigen peptide at amino acids 578 to 585 and induces polyomavirus-specific immunity. [O] . Z Berke, S Palmer, T Bergman, 1996

机译：从多瘤病毒阳性肿瘤的H-2Kb分子洗脱的短肽对应于多瘤病毒大T抗原肽的578至585位氨基酸并诱导多瘤病毒特异性免疫。
7. Multiple binding sites for polyomavirus large T antigen within regulatory sequences of polyomavirus DNA [O] . A Cowie, R Kamen 1984

机译：多马病毒DNA调控序列中多粘附位点的多结合位点

Asp-286----Asn-286 in polyomavirus large T antigen relaxes the specificity of binding to the polyomavirus origin.

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