The histopathology of congenital haemangioma and its clinical correlations: a long‐term follow‐up study of 55 cases

组织病理学 病理 免疫组织化学 医学 相伴的 组织病理学检查 染色 平足蛋白 组织学 淋巴系统 生物 内科学
作者
Sophie El Zein,O. Boccara,V. Soupre,André Filipe Vieira,Christine Bodemer,Aurore Coulomb,Michel Wassef,S. Fraitag
出处
期刊:Histopathology [Wiley]
卷期号:77 (2): 275-283 被引量:23
标识
DOI:10.1111/his.14114
摘要

Aims Congenital haemangiomas (CHs) can be subdivided into different subtypes [rapidly involuting CHs (RICHs), non‐involuting CHs (NICHs), and partially involuting CHs (PICHs)]. During the first few days of life, RICHs may be associated with transient but sometimes marked thrombocytopenia. We sought to assess the histological aspects and clinicopathological correlations of the three subtypes. Methods and results We assessed the histopathological features of 10 RICHs, 25 NICHs, and 20 PICHs, described the patients’ long‐term clinical outcomes, and assessed clinicopathological correlations. All CHs were located in the dermis and hypodermis, and comprised both capillary lobules (with three distinct histopathological patterns) and extralobular large vessels. Most of the extralobular vessels were abnormal veins and abnormal lymphatic vessels. We did not observe significant correlations between the CH subtype, the histopathological pattern, and the time of the histopathological assessment. Interestingly, unexpected intralobular expression of podoplanin was found in neonatal biopsies of five RICHs and PICHs. Four of these five patients had concomitant thrombocytopenia. The podoplanin staining intensity decreased over time as the thrombocytopenia resolved and the tumour shrank. Conclusion The histopathological features were similar in all three subtypes of CH, and were related to the time since disease onset; we consider that RICH, PICH and NICH form a single entity and differ only in their involuting potential. Along with the transient expression of intralobular podoplanin observed in some specimens from the newborn, the lobular architecture might lead to misdiagnosis of tufted haemangioma or kaposiform haemangioendothelioma.

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