Timing of Histological Distal Villous Fetal Vascular Malperfusion in the Placenta: Clinical Significance and Placental Features.

IF 1.1 4区 医学 Q4 MEDICAL LABORATORY TECHNOLOGY Annals of clinical and laboratory science Pub Date : 2024-05-01
Jerzy Stanek
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引用次数: 0

Abstract

Objective: This retrospective analysis compares the diagnostic value of placental large vessel (global, partial) and distal villous (complete, segmental) fetal vascular malperfusion (FVM), remote/established, recent and on-going.

Methods: 24 independent abnormal clinical and 46 placental phenotypes were retrospectively statistically analyzed among 1002 consecutive cases, mostly with congenital anomalies in which CD34 immunostaining was performed. Group A: 398 cases without distal FVM and none or up to two large vessels FVM lesions. Group B: 221 cases with distal villous FVM without clustered endothelial fragmentation by CD34 immunostain. Group C: 145 cases with clustered endothelial fragmentation by CD34 immunostain but no clustered sclerotic or mineralized distal villi. Group D: 163 cases with coexistence of distal villous lesions of Group B and Group C. Group E: 75 cases with three or four lesions of large vessel FVM, but no distal villous FVM lesions.

Results: Established and/or remote FVM had clinical/placental associations similar to those of recent FVM, but on-going FVM was most commonly high grade and associated with preterm pregnancies, stillbirth, and fetal growth restriction. Large vessel FVM usually occurs in advanced third trimester pregnancies with fetal congenital anomalies, villitis of unknown etiology, and intervillous thrombi but no direct association with abnormal fetal condition.

Conclusion: FVM was the most common pattern of placental injury in this material. Proximal FVM was more common than distal FVM, suggesting the sequence of occurrence and the likely umbilical cord compression etiology. CD34 immunostaining doubles the sensitivity of placental examination and frequently upgrades the FVM, making it an important adjunct to placental histology.

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胎盘组织学远端绒毛胎儿血管灌注不良的时间:临床意义和胎盘特征。
目的这项回顾性分析比较了胎盘大血管(整体性、部分性)和远端绒毛(完全性、节段性)胎儿血管灌注不良(FVM)的诊断价值,包括远端/已建立的、近期的和正在进行的。方法:对 1002 例连续病例中的 24 种独立异常临床表型和 46 种胎盘表型进行了回顾性统计分析,这些病例大多为先天性畸形,并进行了 CD34 免疫染色。A 组:398 例无远端胎盘早剥,无或最多有两个大血管胎盘早剥病灶。B 组:221 例有远端绒毛状 FVM,但 CD34 免疫印迹显示没有成簇的内皮碎裂。C 组:145 例病例,CD34 免疫印迹显示内皮碎裂成簇,但远端绒毛无硬化或矿化成簇。D 组E组:75例有3个或4个大血管FVM病变,但无远端绒毛FVM病变:结果:已形成和/或远端大血管胎盘早剥与近期大血管胎盘早剥的临床/胎盘关系相似,但正在形成的大血管胎盘早剥最常见的是高级别,与早产、死胎和胎儿生长受限有关。大血管胎盘早剥通常发生在孕晚期,伴有胎儿先天性畸形、病因不明的绒毛膜炎和绒毛间血栓,但与胎儿异常状况无直接关联:结论:胎盘早剥是本研究中最常见的胎盘损伤模式。结论:胎盘早剥是该样本中最常见的胎盘损伤模式,近端胎盘早剥比远端胎盘早剥更常见,这表明了胎盘早剥的发生顺序以及可能的脐带压迫病因。CD34 免疫染色可使胎盘检查的灵敏度提高一倍,并经常提升 FVM 的等级,使其成为胎盘组织学的重要辅助手段。
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来源期刊
Annals of clinical and laboratory science
Annals of clinical and laboratory science 医学-医学实验技术
CiteScore
1.60
自引率
0.00%
发文量
112
审稿时长
6-12 weeks
期刊介绍: The Annals of Clinical & Laboratory Science welcomes manuscripts that report research in clinical science, including pathology, clinical chemistry, biotechnology, molecular biology, cytogenetics, microbiology, immunology, hematology, transfusion medicine, organ and tissue transplantation, therapeutics, toxicology, and clinical informatics.
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