Establishment of a Diamond‐Blackfan anemia like model in zebrafish

Author:

Ling Yiming1,Wu Jiaye1,Liu Yushi1,Meng Panpan1,Sun Ying1,Zhao Dejian2ORCID,Lin Qing1ORCID

Affiliation:

1. The Innovation Centre of Ministry of Education for Development and Diseases, School of Medicine South China University of Technology Guangzhou China

2. Guangdong Provincial Center for Disease Control and Prevention Guangzhou China

Abstract

AbstractBackgroundAnemia is defined as a lack of erythrocytes, low hemoglobin levels, or abnormal erythrocyte morphology. Diamond‐Blackfan anemia (DBA) is a rare and severe congenital hypoplastic anemia that occurs due to the dominant inheritance of a ribosomal protein gene mutation. Even rarer is a case described as Diamond‐Blackfan anemia like (DBAL), which occurs due to a loss‐of‐function EPO mutation recessive inheritance. The effective cures for DBAL are bone marrow transfusion and treatment with erythropoiesis‐stimulating agents (ESAs). To effectively manage the condition, construction of DBAL models to identify new medical methods or screen drugs are necessary.ResultsHere, an epoa‐deficient mutant zebrafish called epoaszy8 was generated to model DBAL. The epoa‐deficiency in zebrafish caused developmental defects in erythroid cells, leading to severe congenital anemia. Using the DBAL model, we validated a loss‐of‐function EPO mutation using an in vivo functional analysis and explored the ability of ESAs to alleviate congenital anemia.ConclusionsTogether, our study demonstrated that epoa deficiency in zebrafish leads to a phenotype resembling DBAL. The DBAL zebrafish model was found to be beneficial for the in vivo assessment of patient‐derived EPO variants with unclear implications and for devising potential therapeutic approaches for DBAL.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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