A Novel PTPRQ c.3697del Variant Causes Autosomal Dominant Progressive Hearing Loss in Both Humans and Mice.

IF 2.9 3区 医学 Q2 GENETICS & HEREDITY
Yaqi Zhou, Na Yin, Lingchao Ji, Xiaochan Lu, Weiqiang Yang, Weiping Ye, Wenhui Du, Ya Li, Hongyi Hu, Xueshuang Mei
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引用次数: 0

Abstract

PTPRQ plays an important role in the development of inner ear hair cell stereocilia. While many autosomal recessive variants in PTPRQ have been identified as the pathogenic cause for nonsyndromic hearing loss (DFNB84A), so far only one autosomal dominant PTPRQ variant, c.6881G>A (p.Trp2294*), has been reported for late-onset, mild-to-severe hearing loss (DFNA73). By using targeted next-generation sequencing, this study identified a novel PTPRQ truncating pathogenic variant, c.3697del (p.Leu1233Phefs*11), from a Chinese Han family that co-segregated with autosomal dominant, postlingual, progressive hearing loss. A Ptprq-3700del knock-in mouse model was generated by CRISPR-Cas9 and characterized for its hearing function and inner ear morphology. While the homozygous knock-in mice exhibit profound hearing loss at all frequencies at the age of 3 weeks, the heterozygous mutant mice resemble the human patients in mild, progressive hearing loss from age 3 to 12 weeks, primarily affecting high frequencies. At this stage, the homozygous knock-in mice have a normal hair cell count but disorganized stereocilia. Cochlear proteosome analysis of the homozygous mutant mice revealed differentially expressed genes and pathways involved in oxidative phosphorylation, regulation of angiogenesis and synaptic vesicle cycling. Our study provides a valuable animal model for further functional studies of the pathogenic mechanisms underlying DFNA73.

新型 PTPRQ c.3697del 变体导致人类和小鼠常染色体显性进行性听力损失。
PTPRQ 在内耳毛细胞立体纤毛的发育过程中发挥着重要作用。PTPRQ 的许多常染色体隐性变体已被确定为非综合征性听力损失(DFNB84A)的致病原因,但迄今为止,只有一个常染色体显性 PTPRQ 变体,即 c.6881G>A (p.Trp2294*),被报道为迟发、轻度至重度听力损失(DFNA73)的致病原因。通过使用靶向下一代测序技术,本研究从一个中国汉族家庭中发现了一个新型 PTPRQ 截断致病变体 c.3697del (p.Leu1233Phefs*11),该变体与常染色体显性、舌后遗、进行性听力损失共分离。研究人员通过 CRISPR-Cas9 技术生成了 Ptprq-3700del 基因敲入小鼠模型,并对其听力功能和内耳形态进行了鉴定。同基因敲入小鼠在 3 周龄时表现出所有频率的深度听力损失,而杂合子突变小鼠则与人类患者相似,在 3 至 12 周龄期间表现出轻度、进行性听力损失,主要影响高频率。在这一阶段,同源基因敲入小鼠的毛细胞数量正常,但立体纤毛紊乱。对同源突变小鼠耳蜗蛋白质组的分析表明,涉及氧化磷酸化、血管生成调控和突触囊泡循环的基因和通路有不同表达。我们的研究为进一步研究 DFNA73 的致病机制提供了一个宝贵的动物模型。
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来源期刊
Clinical Genetics
Clinical Genetics 医学-遗传学
CiteScore
6.50
自引率
0.00%
发文量
175
审稿时长
3-8 weeks
期刊介绍: Clinical Genetics links research to the clinic, translating advances in our understanding of the molecular basis of genetic disease for the practising clinical geneticist. The journal publishes high quality research papers, short reports, reviews and mini-reviews that connect medical genetics research with clinical practice. Topics of particular interest are: • Linking genetic variations to disease • Genome rearrangements and disease • Epigenetics and disease • The translation of genotype to phenotype • Genetics of complex disease • Management/intervention of genetic diseases • Novel therapies for genetic diseases • Developmental biology, as it relates to clinical genetics • Social science research on the psychological and behavioural aspects of living with or being at risk of genetic disease
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