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四例慢性髓性白血病儿童在伊马替尼治疗期间接种活减毒疫苗。

Vaccination With Live Attenuated Vaccines in Four Children With Chronic Myeloid Leukemia While on Imatinib Treatment.

机构信息

Department of Pediatric Hematology and Oncology, Medical School Hannover, Hanover, Germany.

Department of Pediatric Hematology and Oncology, University Hospital Erlangen, Erlangen, Germany.

出版信息

Front Immunol. 2020 Apr 17;11:628. doi: 10.3389/fimmu.2020.00628. eCollection 2020.

Abstract

Chronic myeloid leukemia (CML) in childhood and adolescence is a rare malignancy that can successfully be treated with the tyrosine kinase inhibitor (TKI) imatinib. According to the current experience, treatment is necessary for years and, in the majority of cases, a lifelong approach is required to control the malignant disease. To what extent imatinib causes immunosuppression in different age cohorts is a controversial discussion. According to general medical recommendations, live vaccines are contraindicated in individuals treated with imatinib. However, a recent increase in the number of globally reported cases of measles has been observed and continues to rise. Due to the high contagiousness of the virus, near-perfect vaccination coverage (herd immunity of 93 to 95%) is required to effectively protect against measles resurgence-a scenario that is not realistic in many countries. When four teenagers with CML (median age 13 years, range 12-15) who were enrolled into pediatric trial CML-paed II while on imatinib treatment (median treatment duration 36 months, range 11-84) were identified without protective measles and/or varicella titers, we carefully balanced the risks of a live vaccination under immunosuppressive TKI medication against the benefit of being protected. The patients underwent live vaccination with the live attenuated vaccines M-M-RVAX Pro and Varivax simultaneously (Patient #1), Priorix and Varilix consecutively (Patient #2), and Priorix (Patients #3 and #4). While the first three patients were vaccinated while receiving TKI therapy, treatment with imatinib was interrupted in patient #4 for 1 week prior and 2 weeks after vaccination. Patients #1 and #3 reacted with stable long-term seroconversion. In Patient #2, serum titer conversion against measles and varicella could not be demonstrated and thus revaccination with Priorix and Varilix was performed 3 years later. However, protective titers did not develop or were lost again. Patient #4 also lost protective titers against measles when assessed 10 months after vaccination, but revaccination resulted in stable seroprotective titers over 12 months after the last vaccination during ongoing imatinib treatment. We conclude that in all patients, the safety of live vaccines could be documented, as no acute or late adverse events were observed. However, in line with observations that memory B-cells are lost under exposure to imatinib, revaccination may become necessary (two out of four patients in this small series lost their seroprotection). Considering that the number of cases is very small, we also suggest some criteria for decision-making regarding live vaccinations of CML patients treated with imatinib.

摘要

儿童和青少年慢性髓性白血病(CML)是一种罕见的恶性肿瘤,可以成功地用酪氨酸激酶抑制剂(TKI)伊马替尼治疗。根据目前的经验,需要多年的治疗,在大多数情况下,需要终身治疗来控制恶性疾病。伊马替尼在不同年龄组中引起免疫抑制的程度是一个有争议的讨论。根据一般医学建议,正在接受伊马替尼治疗的个体禁忌使用活疫苗。然而,最近观察到并持续增加了全球报告的麻疹病例数。由于该病毒具有高度传染性,需要接近完美的疫苗接种覆盖率(93%至 95%的群体免疫)才能有效地预防麻疹卷土重来——在许多国家,这种情况并不现实。当发现正在接受伊马替尼治疗的儿科试验 CML-paed II 入组的 4 名 CML 青少年(中位年龄 13 岁,范围 12-15 岁)没有保护性麻疹和/或水痘滴度时,我们仔细权衡了在免疫抑制性 TKI 药物下进行活疫苗接种的风险与获得保护的益处。患者同时接受活减毒疫苗 M-M-RVAX Pro 和 Varivax(患者#1)、Priorix 和 Varilix 连续接种(患者#2)以及 Priorix(患者#3 和#4)。在前 3 名患者接受 TKI 治疗的同时进行了疫苗接种,而患者#4 在接种前 1 周和接种后 2 周暂停了伊马替尼治疗。患者#1 和#3 反应稳定,长期血清转化。然而,患者#2 未能证明对麻疹和水痘的血清滴度转换,因此在 3 年后再次进行了 Priorix 和 Varilix 接种。然而,保护性滴度没有再次产生或再次丢失。患者#4 在接种后 10 个月时也失去了对麻疹的保护性滴度,但在持续接受伊马替尼治疗期间的最后一次接种后 12 个月,再次接种导致稳定的血清保护滴度。我们得出结论,在所有患者中,活疫苗的安全性均可得到证实,因为未观察到急性或迟发性不良事件。然而,与观察到的伊马替尼暴露下记忆 B 细胞丢失一致,可能需要再次接种疫苗(本小系列中有 4 名患者中的 2 名失去了血清保护)。鉴于病例数量非常少,我们还建议了一些决策标准,用于决定接受伊马替尼治疗的 CML 患者的活疫苗接种。

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