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高哌可酸血症在泽尔韦格综合征中的意义。

The significance of hyperpipecolatemia in Zellweger syndrome.

作者信息

Dancis J, Hutzler J

出版信息

Am J Hum Genet. 1986 May;38(5):707-11.

Abstract

The plasma pipecolic acid concentration in two newborn infants with Zellweger syndrome at ages 4 and 10 days were 7.8 and 7.7 microM. Reported concentrations from this laboratory for normal newborn infants averaged 12 microM +/- 5.6 (SD). Both patients had the facies and severe hypotonia characteristic of the disease. Autopsy examination at age 6 days in one of these patients revealed the developmental microscopic abnormalities in brain, liver, and kidney that are associated with Zellweger syndrome. In three additional patients ages 3 1/2 weeks, 2 months, and 2 months, the pipecolic acid concentrations were 15, 17, and 25 microM. The concentrations increased to distinctly pathological levels on subsequent assays at a later age. It is concluded that the hyperpipecolatemia in Zellweger syndrome occurs postpartum and that the plasma concentrations may not be diagnostic early in life. The major manifestations of the disease, already evident at birth, cannot be attributed to pipecolatemia. Currently available data do not exclude the possibility of pipecolic acid accumulation in the brain where it has been reported to be a major metabolite of lysine. Hyperpipecolatemia of considerable degree is also consistently found in familial hyperlysinemia where it appears to be benign.

摘要

两名患有泽韦格综合征的新生儿在4天和10天时的血浆哌可酸浓度分别为7.8和7.7微摩尔/升。本实验室报告的正常新生儿的平均浓度为12微摩尔/升±5.6(标准差)。两名患者均具有该疾病典型的面容和严重肌张力减退。其中一名患者在6天时进行的尸检显示,其脑、肝和肾存在与泽韦格综合征相关的发育性微观异常。另外三名年龄分别为3.5周、2个月和2个月的患者,其哌可酸浓度分别为15、17和25微摩尔/升。在随后的较晚年龄检测中,这些浓度升高至明显的病理水平。结论是,泽韦格综合征中的高哌可酸血症发生在产后,血浆浓度在生命早期可能无法用于诊断。该疾病在出生时就已明显的主要表现不能归因于高哌可酸血症。目前可得的数据并不排除哌可酸在大脑中积累的可能性,据报道它是赖氨酸的主要代谢产物。在家族性高赖氨酸血症中也始终发现有相当程度的高哌可酸血症,而这种情况似乎是良性的。

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L-pipecolaturia in Zellweger syndrome.
Biochim Biophys Acta. 1986 Jun 19;882(2):254-7. doi: 10.1016/0304-4165(86)90162-5.

本文引用的文献

3
The determination of pipecolic acid: method and results of hospital survey.
Clin Chim Acta. 1983 Feb 28;128(1):75-82. doi: 10.1016/0009-8981(83)90057-8.
10
Pipecolic acid pathway: the major lysine metabolic route in the rat brain.
Biochem Biophys Res Commun. 1976 Mar 8;69(1):174-80. doi: 10.1016/s0006-291x(76)80288-4.

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