新生儿高酪氨酸血症的诊断误区:病例报告

K. Khalid, Mohd Fazrul Shafiq Kamarudzaman, Siti Nurwani Ahmad Ridzuan, Nurul Izzati Hamzan, Norzahidah Khalid, Noor Hafizah Hassan
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摘要

高酪氨酸血症源于酪氨酸代谢异常。获得性高酪氨酸血症比遗传性高酪氨酸血症更为常见,通常在生化检测中表现为继发性病因。在此,我们介绍一例不寻常的病例,一名出生 16 天的女婴被筛查出患有先天性代谢异常(IEM)。她出现黄疸、肌张力低下、嗜睡,检查时发现肝脏肿大。她因多器官受累的败血症接受治疗,需要加强静脉注射抗生素和辅助通气。她的干血斑(DBS)显示酪氨酸中度升高(408umol/L,N:10-182),Phe:Tyr比值较低(0.15mmol/L,N:0.32-3.45)。血浆氨基酸显示为 807 毫摩尔/升(N:5-167)的孤立高酪氨酸血症,其他肝脏代谢物轻度升高,但不明显。尿液有机酸中未见琥珀酰丙酮峰值,尽管 DBS、血浆氨基酸和临床表现均有特征性结果,但遗传性酪氨酸血症 I 型的诊断可能性较低。两周后再次进行 IEM 筛查,发现 DBS 和血浆氨基酸均无诊断结果,而败血症已缓解,临床症状也有所改善。本病例强调了对遗传性酪氨酸血症高度怀疑的患儿进行不相容生化检测所面临的挑战。在我们的病例中,反复筛查排除了遗传性酪氨酸血症,提示最初的高酪氨酸血症可能是由于肝功能异常和负责酪氨酸分解代谢的肝酶活性受损所致。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Diagnostic pitfalls in neonatal hypertyrosinemia: a case report
Hypertyrosinemia results from abnormality in tyrosine metabolism. Acquired hypertyrosinemia is notably more common than inherited types and typically presents with profile suggestive of secondary aetiology on biochemical testing. Herein, we present an unusual case of a day 16-of-life baby girl who was screened for inborn errors of metabolism (IEM). She presented with jaundice, hypotonia, lethargy and had hepatomegaly on examination. She was treated for sepsis with multiorgan involvement, requiring escalation of intravenous antibiotics and assisted ventilation. Her dried blood spot (DBS) showed moderate elevation of tyrosine (408umol/L, N:10-182) with low Phe:Tyr ratio (0.15mmol/L, N:0.32-3.45). Plasma amino acid showed isolated hypertyrosinemia at 807mmol/L (N:5-167) with mild, non-significant elevations of other liver metabolites. No succinylacetone peak seen with urine organic acids, making the diagnosis of inherited Tyrosinemia type I less likely despite the characteristic findings from DBS, plasma amino acids, and presenting clinical signs. Repeated IEM screening two weeks later revealed a non-diagnostic profile across both DBS and plasma amino acids in light of resolving sepsis and clinical improvement. This case highlights the challenges associated with incompatible biochemical testing in a child with a high index of suspicion for inherited Tyrosinemia. In our case, repeated screening ruled out inherited Tyrosinemia, suggesting the initial picture of hypertyrosinemia to be likely due to liver dysfunction and impaired activity of liver enzymes that are responsible for tyrosine catabolism.
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