Prenatal phenotype of PNKP-related microcephaly, seizures, and developmental delay: A case report and literature review.

IF 1.3 4区医学 Q2 MEDICINE, GENERAL & INTERNAL

Medicine Pub Date : 2025-01-17 DOI:10.1097/MD.0000000000041300

Jin-Long Xie, Chun-Yan Jiang, Ping-Ping Sun, Yan Zhang, Na Sun, Su-Xian Luan

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引用次数: 0

Abstract

Rationale: Microcephaly, epilepsy, and developmental delay (MCSZ) is a rare neurodevelopmental disorder associated with autosomal recessive inheritance of mutations in the polynucleotide kinase 3'-phosphatase (PNKP) gene. Prompt identification and management are essential, as delayed diagnosis or intervention may result in severe complications or mortality. In this case, prenatal screening in the second trimester detected fetal microcephaly with a gradual decline in head circumference, prompting the decision to terminate the pregnancy. Subsequent genetic analysis of the fetal tissue confirmed the presence of compound heterozygous mutations in the PNKP gene.

Patient concerns: The patient, a 34-year-old remarried female with no history of consanguineous marriage, underwent 2 mid-trimester termination procedures due to fetal microcephaly and sought counseling for reproductive assistance.

Diagnoses: The patient's carrier status for PNKP mutations was ascertained through whole-exome sequencing of the termination tissue and molecular genetic testing for monogenic disorders. The terminated fetus was diagnosed with MCSZ, a condition associated with compound heterozygous mutations in the PNKP gene.

Interventions: Fetal microcephaly was identified via mid-trimester prenatal ultrasound, leading to the termination of the pregnancy during the same trimester. Subsequent genetic analysis of the immediate family revealed compound heterozygous mutations in the PNKP gene as the underlying cause of MCSZ. Genetic counseling was provided, followed by 1 cycle of preimplantation genetic testing for monogenic.

Outcomes: The patient carried the heterozygous c.1188 + 1G > A PNKP mutation, whereas her husband carried the heterozygous c.976G > A PNKP mutation. The fetus was found to have compound heterozygous mutations c.976G > A and c.1188 + 1G > A. After counseling, the couple underwent 1 cycle of preimplantation genetic testing for monogenic, unfortunately, no pregnancy occurred after the 2 embryos were transferred.

Lessons: MCSZ, a condition caused by PNKP mutations, is exceedingly rare. Women with a history of adverse pregnancy outcomes should undergo close monitoring during prenatal checkups. If fetal microcephaly is detected, it is essential to strictly follow obstetric guidelines for prenatal care, such as comprehensive cranial magnetic resonance imaging and genetic testing for confirmation. Avoidance of consanguineous marriages is advised. Early detection and timely intervention are key to preventing adverse pregnancy outcomes.

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pnkp相关的小头畸形、癫痫发作和发育迟缓的产前表型：一个病例报告和文献复习。

理由：小头畸形、癫痫和发育迟缓（MCSZ）是一种罕见的神经发育障碍，与多核苷酸激酶3′-磷酸酶（PNKP）基因突变的常染色体隐性遗传有关。及时识别和处理至关重要，因为延迟诊断或干预可能导致严重并发症或死亡。在这种情况下，产前筛查在妊娠中期发现胎儿小头畸形，头围逐渐下降，促使决定终止妊娠。随后对胎儿组织的遗传分析证实了PNKP基因中存在复合杂合突变。患者关注：患者34岁，再婚女性，无近亲婚姻史，因胎儿小头畸形接受了两次中期终止妊娠手术，并寻求生殖协助咨询。诊断：通过终止组织的全外显子组测序和单基因疾病的分子基因检测来确定患者PNKP突变的携带者状态。被终止的胎儿被诊断为MCSZ，这是一种与PNKP基因的复合杂合突变有关的疾病。干预措施：通过妊娠中期产前超声发现胎儿小头畸形，导致在同一妊娠期终止妊娠。随后对直系亲属的遗传分析显示，PNKP基因的复合杂合突变是MCSZ的潜在原因。提供遗传咨询，然后进行1个周期的单基因植入前基因检测。结果：患者携带杂合型c.1188 + 1G > A PNKP突变，而其丈夫携带杂合型c.976G > A PNKP突变。发现胎儿具有复合杂合突变c.976G > A和c.1188 + 1G > A。经咨询后，夫妇俩进行了1个周期的单基因植入前基因检测，不幸的是，两个胚胎移植后没有怀孕。经验教训：MCSZ是一种由PNKP突变引起的疾病，非常罕见。有不良妊娠结局史的妇女应在产前检查时密切监测。如果检测到胎儿小头畸形，必须严格遵守产科产前护理指南，例如全面的颅脑磁共振成像和基因检测以进行确认。建议避免近亲结婚。早期发现和及时干预是预防不良妊娠结局的关键。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Medicine 医学-医学：内科

CiteScore

2.80

自引率

0.00%

发文量

4342

审稿时长

>12 weeks

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