Varma Anshu, Bolotin Shelly, De Serres Gaston, Didierlaurent Arnaud M, Earle Kristen, Frey Kurt, Hahné Susan, Kapelus Daniel, Krause L Kendall, McCarthy Kevin, Moss William J, Orenstein Walter A, van Binnendijk Rob, Vittrup Dorthe Maria, Voysey Merryn, Woudenberg Tom, Bar-Zeev Naor, Bose Anindya S, Hombach Joachim, Mulders Mick N, Lochlainn Laura Nic, Suwintono Kezia, Feikin Daniel R, Crowcroft Natasha S
Department of Immunization, Vaccines, and Biologicals World Health Organization, Geneva, Switzerland.
Centre for Vaccine Preventable Diseases, Dalla Lana School of Public Health, and Department of Laboratory Medicine and Pathobiology, University of Toronto, Toronto, Canada.
Vaccine. 2025 May 31;57:127187. doi: 10.1016/j.vaccine.2025.127187. Epub 2025 May 14.
Measles is one of the most contagious vaccine preventable diseases, causing severe complications and deaths globally. While vaccination with a measles-containing vaccine (MCV) has prevented millions of measles deaths, recent trends, especially from low- and middle-income countries, are discouraging. Measles cases have increased since 2021 as MCV coverage has decreased; and an estimated 107,500 measles deaths, mostly in children under-five years, occurred in 2023. Thus, a renewed focus on proven and innovative strategies to control measles is needed. The World Health Organization (WHO) recommends a first MCV dose administered at 9-15 months of age (routine MCV1), however MCV1 below 9 months of age (early MCV1) may increase vaccination coverage because uptake of all vaccines tends to be higher the younger the child, and this might protect vulnerable infants earlier in life. However, due to concerns about possible reduced vaccine performance, early MCV1 is not routinely recommended by WHO. WHO hosted an informal technical consultation on December 6-7, 2023, in Geneva, Switzerland to evaluate recent evidence on early MCV1 and identify evidence gaps for policy making. The recent evidence suggests a robust humoral immune response shortly after early MCV1 at 5-8 months of age. Immune blunting of a routine second MCV dose (e.g., MCV2) after early MCV1 was not demonstrated in the presented data. However, 3-7 years after MCV1, children receiving early MCV1 had lower measles antibodies than children receiving routine MCV1, suggesting faster waning of immunity. The totality of evidence on immune blunting remains inconsistent. Meeting participants thought more data are needed before revisiting WHO's current recommendation for a potential revision. Evidence gaps include: understanding measles disease burden and severity in infants; early MCV1 effectiveness and duration; vaccine-induced cellular immunogenicity; whether measles in infants is acquired from other infants or older children or adults; and blunting of routine MCV2. Addressing evidence gaps through targeted studies and measles outbreak investigations, as well as evaluations of country-level introductions of early MCV1 are warranted. Ensuring high MCV1 and MCV2 coverage remains the priority in measles control.
麻疹是传染性最强的疫苗可预防疾病之一,在全球范围内会引发严重并发症和死亡。虽然接种含麻疹疫苗(MCV)已预防了数百万例麻疹死亡,但近期趋势,尤其是来自低收入和中等收入国家的趋势,令人沮丧。自2021年以来,随着MCV接种覆盖率下降,麻疹病例有所增加;2023年估计有107,500例麻疹死亡,其中大多数是五岁以下儿童。因此,需要重新关注已证实的和创新的麻疹控制策略。世界卫生组织(WHO)建议在9至15月龄接种第一剂MCV(常规MCV1),然而9月龄以下接种MCV1(早期MCV1)可能会提高疫苗接种覆盖率,因为儿童越小,所有疫苗的接种率往往越高,这可能会在生命早期保护易感染婴儿。然而,由于担心疫苗效果可能降低,WHO不常规推荐早期MCV1。WHO于2023年12月6日至7日在瑞士日内瓦举办了一次非正式技术磋商会,以评估关于早期MCV1的最新证据,并确定政策制定方面的证据空白。最新证据表明,在5至8月龄接种早期MCV1后不久会产生强大的体液免疫反应。现有数据未显示早期MCV1后常规第二剂MCV(如MCV2)的免疫减弱情况。然而,在接种MCV1后3至7年,接种早期MCV1的儿童的麻疹抗体低于接种常规MCV1的儿童,这表明免疫力下降更快。关于免疫减弱的全部证据仍然不一致。与会者认为,在重新审视WHO目前的建议以进行可能的修订之前,需要更多数据。证据空白包括:了解婴儿中的麻疹疾病负担和严重程度;早期MCV1的有效性和持续时间;疫苗诱导的细胞免疫原性;婴儿麻疹是否从其他婴儿、年长儿童或成人处获得;以及常规MCV2的免疫减弱情况。通过有针对性的研究和麻疹疫情调查,以及对国家层面引入早期MCV1的评估来填补证据空白是必要的。确保高MCV1和MCV2接种覆盖率仍然是麻疹控制的优先事项。
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