共查询到7条相似文献,搜索用时 0 毫秒
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Stephen J. Simko MD Huy D. Tran MD Jeremy Jones MD Mrinalini Bilgi MS Lynda Kwon Beaupin MD Don Coulter MD Timothy Garrington MD Timothy L. McCavit MD Colin Moore MD Francisco Rivera‐Ortegón MD Linda Shaffer MD Linda Stork MD Lucie Turcotte MD Esperanza C. Welsh MD M. John Hicks MD PhD DDS Kenneth L. McClain MD PhD Carl E. Allen MD PhD 《Pediatric blood & cancer》2014,61(3):479-487
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Hammill AM Wentzel M Gupta A Nelson S Lucky A Elluru R Dasgupta R Azizkhan RG Adams DM 《Pediatric blood & cancer》2011,57(6):1018-1024
Background
Vascular anomalies comprise a diverse group of diagnoses. While infantile hemangiomas are common, the majority of these conditions are quite rare and have not been widely studied. Some of these lesions, though benign, can impair vital structures, be deforming, or even become life‐threatening. Vascular tumors such as kaposiform hemangioendotheliomas (KHE) and complicated vascular malformations have proven particularly difficult to treat.Procedure
Here we retrospectively evaluate a series of six patients with complicated, life‐threatening vascular anomalies who were treated with the mTOR inhibitor sirolimus for compassionate use at two centers after failing multiple other therapies.Results
These patients showed significant improvement in clinical status with tolerable side effects.Conclusions
Sirolimus appears to be effective and safe in patients with life‐threatening vascular anomalies and represents an important tool in treating these diseases. These findings are currently being further evaluated in a Phase II safety and efficacy trial. Pediatr Blood Cancer 2011; 57: 1018–1024. © 2011 Wiley‐Liss, Inc. 相似文献4.
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Nanda Kerkar Raffaella A. Morotti Rebecca P. Madan Benjamin Shneider Betsy C. Herold Christina Dugan Tamir Miloh Ilhan Karabicak James A. Strauchen Sukru Emre 《Pediatric transplantation》2010,14(4):504-511
Kerkar N, Morotti RA, Madan RP, Shneider B, Herold BC, Dugan C, Miloh T, Karabicak I, Strauchen JA, Emre S. The changing face of post‐transplant lymphoproliferative disease in the era of molecular EBV monitoring.Pediatr Transplantation 2010: 14:504–511. © 2010 John Wiley & Sons A/S. Abstract: Pediatric PTLD is often associated with primary EBV infection and immunosuppression. The aim was to retrospectively review the spectrum of histologically documented PTLD for two time intervals differentiated by changes in use of molecular EBV monitoring. Eleven of 146 patients (7.5%) in 2001–2005 (Era A) and 10 of 92 (10.9%) in 1993–1997 (Era B) were diagnosed with PTLD. The median age at liver transplantation (0.8 and 0.9 yr, respectively) and the median duration between liver transplant and diagnosis of PTLD (0.6 and 0.7 yr, respectively) were similar in both eras. However, patients in Era A presented with significantly less advanced histological disease compared to patients in Era B (p = 0.03). Specifically, nine patients (82%) in Era A had Pl hyperplasia/polymorphic PTLD, whereas in Era B, six had advanced histological disease (five monomorphic and one unclassified). Three transplant recipients in Era B died secondary to PTLD, whereas there were no PTLD‐related deaths in Era A (p = 0.03). Heightened awareness of risk for PTLD, alterations in baseline immunosuppression regimens, implementation of molecular EBV monitoring, pre‐emptive reduction in immunosuppression and improved therapeutic options may have all contributed to a milder PTLD phenotype and improved clinical outcomes. 相似文献