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Impact of sirolimus treatment for refractory kaposiform hemangioendothelioma with exacerbation of the disease 10 years after initial diagnosis

机译:西罗莫司治疗对难治性卡波西氏型血管内皮瘤的影响-初步诊断后10年加重病情

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摘要

We describe our experience with a 12 year-old girl with kaposiform hemangioendothelioma accompanied by Kasabach–Merritt phenomenon with exacerbation of the disease 10 years after the initial diagnosis. Kaposiform hemangioendothelioma infiltrated into the subcutaneous tissue of the facial skin with deterioration of coagulopathy despite conventional therapies including corticosteroid, vincristine, and propranolol. Sirolimus, a mammalian target of rapamycin inhibitor, produced rapid and dramatic improvement of the Kasabach–Merritt phenomenon and kaposiform hemangioendothelioma shrinkage. Eventually, multifocal lesions of kaposiform hemangioendothelioma disappeared on the images of magnetic resonance imaging and have remained in remission for 27 months after sirolimus cessation. We demonstrated that the AKT/mammalian target of rapamycin signaling pathway played a pivotal role in the kaposiform hemangioendothelioma growth. Sirolimus must be a strong candidate for molecular therapy targeting kaposiform hemangioendothelioma.
机译:我们描述了我们对一名12岁的卡波西氏样血管内皮瘤伴有卡萨巴赫-梅里特现象的女孩的经历,该病在最初诊断后10年就加重了病情。尽管常规疗法包括皮质类固醇,长春新碱和普萘洛尔,但是卡波西氏型血管内皮瘤浸润到面部皮肤的皮下组织中,伴有凝血病的恶化。西罗莫司是雷帕霉素抑制剂的哺乳动物靶点,可迅速而显着改善卡萨巴赫-梅里特现象和卡波西型血管内皮细胞瘤的缩小。最终,卡波西氏型血管内皮瘤的多灶性病变在磁共振成像图像上消失,并且在西罗莫司停止治疗后已缓解了27个月。我们证明了雷帕霉素信号传导途径的AKT /哺乳动物靶标在卡波西型血管内皮瘤生长中起着关键作用。西罗莫司必须是针对卡波西型血管内皮瘤的分子疗法的有力候选者。

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