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Computational Studies of the Structural Basis of Human RPS19 Mutations Associated With Diamond-Blackfan Anemia
被引:4
作者:

An, Ke
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Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China

Zhou, Jing-Bo
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Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China

Xiong, Yao
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Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China

Han, Wei
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Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China

Wang, Tao
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机构:
Shenzhen Bay Lab, Shenzhen, Peoples R China Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China

Ye, Zhi-Qiang
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机构:
Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China
Shenzhen Bay Lab, Shenzhen, Peoples R China Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China

Wu, Yun-Dong
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h-index: 0
机构:
Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China
Shenzhen Bay Lab, Shenzhen, Peoples R China
Peking Univ, Coll Chem & Mol Engn, Beijing, Peoples R China Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China
机构:
[1] Peking Univ, Shenzhen Grad Sch, State Key Lab Chem Oncogenom, Shenzhen, Peoples R China
[2] Shenzhen Bay Lab, Shenzhen, Peoples R China
[3] Peking Univ, Coll Chem & Mol Engn, Beijing, Peoples R China
基金:
中国国家自然科学基金;
关键词:
Diamond-Blackfan Anemia;
RPS19;
missense mutation;
structure stability;
interaction;
pathogenesis;
ribosomopathy;
RIBOSOMAL-PROTEIN S19;
AMINO-ACID-RESIDUES;
GENE;
TOOL;
VISUALIZATION;
CONSERVATION;
RECOGNITION;
PREFERENCES;
STABILITY;
VARIANTS;
D O I:
10.3389/fgene.2021.650897
中图分类号:
Q3 [遗传学];
学科分类号:
071007 ;
090102 ;
摘要:
Diamond-Blackfan Anemia (DBA) is an inherited rare disease characterized with severe pure red cell aplasia, and it is caused by the defective ribosome biogenesis stemming from the impairment of ribosomal proteins. Among all DBA-associated ribosomal proteins, RPS19 affects most patients and carries most DBA mutations. Revealing how these mutations lead to the impairment of RPS19 is highly demanded for understanding the pathogenesis of DBA, but a systematic study is currently lacking. In this work, based on the complex structure of human ribosome, we comprehensively studied the structural basis of DBA mutations of RPS19 by using computational methods. Main structure elements and five conserved surface patches involved in RPS19-18S rRNA interaction were identified. We further revealed that DBA mutations would destabilize RPS19 through disrupting the hydrophobic core or breaking the helix, or perturb the RPS19-18S rRNA interaction through destroying hydrogen bonds, introducing steric hindrance effect, or altering surface electrostatic property at the interface. Moreover, we trained a machine-learning model to predict the pathogenicity of all possible RPS19 mutations. Our work has laid a foundation for revealing the pathogenesis of DBA from the structural perspective.
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