Dual enzyme therapy improves adherence to chemotherapy in a patient with gaucher disease and Ewing sarcoma.

IF 1.2 4区 医学 Q4 HEMATOLOGY Pediatric Hematology and Oncology Pub Date : 2023-05-01 DOI:10.1080/08880018.2022.2124006
Brandon Lucari, Eran Tallis, Vernon Reid Sutton, Timothy Porea
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引用次数: 1

Abstract

This case reports concomitant use of enzyme and substrate reduction therapy to improve chemotherapy adherence in a pediatric patient diagnosed with Ewing sarcoma (ES) and type 1 Gaucher disease (GD). The 17-year-old female presented with 5 months of right knee pain with associated mass on exam. She was diagnosed with ES with pulmonary metastasis. The patient was treated with 17 alternating cycles of vincristine-doxorubicin-cyclophosphamide and ifosfamide and etoposide chemotherapy followed by tumor resection and radiation per standard protocol. As part of her staging work-up, bone marrow biopsy was performed, significant for Gaucher cells. After the second cycle of chemotherapy the patient began to experience severe delays averaging 30 days between cycles compared to 17.29 days observed in Children's Oncology Group data. Given her bone marrow biopsy findings and chemotherapy delays GD screening was obtained and the patient was diagnosed with GD following genetic confirmation. Due to delays in chemotherapy decreasing chance of remission, the patient was referred to Genetics for aggressive management with imiglucerase and eliglustat. After initiation of therapy the period between chemotherapy cycles decreased to 23 days on average, with a 21% increase in platelet count during therapy. The patient was able to complete ES therapy achieving remission. GD is associated with an increased risk of malignancy, as seen in our patient with ES. GD patients experience prolonged hematologic cytopenia during cancer treatment. Combining Enzyme and Substrate Reduction Therapies should be investigated as an option to improve chemotherapy adherence in GD patients.

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双酶治疗提高戈谢病和尤因肉瘤患者的化疗依从性。
本病例报告了一名诊断为尤文氏肉瘤(ES)和1型戈谢病(GD)的儿科患者同时使用酶和底物还原疗法来提高化疗依从性。17岁女性在检查时表现为5个月的右膝疼痛并伴有肿块。她被诊断为ES伴肺转移。患者接受了17个交替周期的长春新碱-阿霉素-环磷酰胺和异环磷酰胺和依托泊苷化疗,然后按照标准方案进行肿瘤切除和放疗。作为分期检查的一部分,进行了骨髓活检,对戈谢氏细胞有重要意义。在第二个化疗周期后,患者开始经历严重的延迟,平均间隔30天,而儿童肿瘤组的数据为17.29天。鉴于她的骨髓活检结果和化疗延迟,进行了GD筛查,并在遗传确认后诊断为GD。由于化疗延迟减少了缓解的机会,患者被转介到遗传学对伊米格鲁酶和依利司他进行积极的管理。治疗开始后,化疗周期之间的时间平均减少到23天,治疗期间血小板计数增加21%。患者能够完成ES治疗并获得缓解。GD与恶性肿瘤的风险增加有关,正如我们的ES患者所见。GD患者在癌症治疗期间经历了长期的血液学细胞减少。应研究联合酶和底物还原治疗作为改善GD患者化疗依从性的一种选择。
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来源期刊
CiteScore
2.60
自引率
5.90%
发文量
71
审稿时长
6-12 weeks
期刊介绍: PHO: Pediatric Hematology and Oncology covers all aspects of research and patient management within the area of blood disorders and malignant diseases of childhood. Our goal is to make PHO: Pediatric Hematology and Oncology the premier journal for the international community of clinicians and scientists who together aim to define optimal therapeutic strategies for children and young adults with cancer and blood disorders. The journal supports articles that address research in diverse clinical settings, exceptional case studies/series that add novel insights into pathogenesis and/or clinical care, and reviews highlighting discoveries and challenges emerging from consortia and conferences. Clinical studies as well as basic and translational research reports regarding cancer pathogenesis, genetics, molecular diagnostics, pharmacology, stem cells, molecular targeting, cellular and immune therapies and transplantation are of interest. Papers with a focus on supportive care, late effects and on related ethical, legal, psychological, social, cultural, or historical aspects of these fields are also appreciated. Reviews on important developments in the field are welcome. Articles from scientists and clinicians across the international community of Pediatric Hematology and Oncology are considered for publication. The journal is not dependent on or connected with any organization or society. All submissions undergo rigorous peer review prior to publication. Our Editorial Board includes experts in Pediatric Hematology and Oncology representing a wide range of academic and geographic diversity.
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