首页> 外文期刊>Journal of Neuropathology and Experimental Neurology: Official Journal of the American Association of Neuropathologists, Inc >Beta-amyloid precursor protein staining in nonhomicidal pediatric medicolegal autopsies.
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Beta-amyloid precursor protein staining in nonhomicidal pediatric medicolegal autopsies.

机译:β-淀粉样蛋白前体蛋白染色在非杀婴性小儿法医学尸检中。

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摘要

Immunohistochemical staining for beta-amyloid precursor protein (betaAPP) has been validated as a marker for axonal injury in adults surviving > or = 2 hours after white matter damage. The significance of betaAPP staining in pediatric brains and spinal cords is not as well established. We evaluated the white matter immunoreactivity for betaAPP from a variety of pediatric medicolegal autopsies: natural disease (non-Sudden Infant Death Syndrome [SIDS]), SIDS, motor vehicle accidents, drowning, near-drowning, overlay, carbon monoxide toxicity, miscellaneous trauma, and mechanical asphyxia. The cases of carbon monoxide toxicity, motor vehicle accidents (death at scene), drowning (with resuscitation), and a natural (non-SIDS) death had no significant white matter staining. The traumatic deaths with a significant survival interval, a variety of natural deaths, the near-drowning case, and surprisingly, all SIDS had detectable betaAPP white matter immunostaining. These results demonstrate that features other than traumatic axonal injury, such as metabolic insults and hypoxic-ischemic injury secondary to vascular compromise, must contribute to betaAPP immunostaining. In addition, we describe a variety of betaAPP-immunoreactive structures not previously reported in the pediatric population. This study illustrates that betaAPP immunostaining enhances detection of a variety of white matter changes, and provides a basis for interpretation of these results.
机译:β-淀粉样蛋白前体蛋白(betaAPP)的免疫组织化学染色已被证实是在白质损伤后存活超过2小时的成年人中轴突损伤的标志物。 βAPP染色在小儿脑和脊髓中的意义还不太清楚。我们评估了各种儿科法医学尸检中βAPP的白质免疫反应性:自然疾病(非猝死婴儿死亡综合症[SIDS]),SIDS,机动车交通事故,溺水,溺水,溺水,覆盖,一氧化碳毒性,其他创伤和机械性窒息。一氧化碳毒性,机动车事故(现场死亡),溺水(有复苏)和自然死亡(非SIDS)的病例均无明显的白质染色。具有重大生存间隔的创伤性死亡,各种自然死亡,濒临死亡的病例,而且令人惊讶的是,所有SIDS均具有可检测到的betaAPP白质免疫染色。这些结果表明,除了创伤性轴索损伤外,其他特征(如代谢损伤和继发于血管损伤的缺氧缺血性损伤)也必须促进betaAPP免疫染色。此外,我们描述了以前在儿科人群中尚未报道的多种betaAPP免疫反应性结构。这项研究表明betaAPP免疫染色增强了对各种白质变化的检测,并为解释这些结果提供了基础。

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