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首页> 外文期刊>The Indian journal of medical research. >A pilot study on parvovirus B19 infection in paediatric haematological malignancies.
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A pilot study on parvovirus B19 infection in paediatric haematological malignancies.

机译:细小病毒B19感染在小儿血液系统恶性肿瘤中的初步研究。

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BACKGROUND & OBJECTIVES: Leukaemia and lymphoma are common paediatric haematological malignancies acquiring human parvovirus B19 (B19) infection. In some studies anaemia has been found in children with acute lymphoblastic leukaemia (ALL) during maintenance therapy and rarely in lymphoma. We studied frequency of B19 infection and its implications in new onset acute leukaemia (mostly ALL) and lymphoma in children. METHODS: Seventy serum samples from 35 children (age <12 yr, 29 males) newly diagnosed with haematological malignancies (on induction therapy) were collected together with 34 controls (solid tumours). Children were examined clinically and for anti-B19 IgM antibodies by quantitative ELISA and B19 DNA by PCR (VP1-VP2) and nested-PCR (VP1 unique). Bone marrow aspirates were examined histopathologically, whenever possible. RESULTS: Of the 35 children, 22 had acute leukaemia while 13 had lymphoma. B19 infection was seen in six (17.1%) of 35 children (5 ALL, 1 NHL), two at diagnosis and four during follow up compared to none in the control. Among five B19 IgM positive ALL (n=18) children, two had B19 genome and two had giant pronormoblasts (lantern cells; but one lacked B19 DNA). Of the 70 serum samples tested, eight (11.4%) had anti-B19 IgM as two children had persistent B19 infection and one showed atypical maculopapular rashes (lower limbs) while 12 (34.3%) had anti-B19 IgG antibodies. B19 infected children had unexplained anaemia (80%), required more blood transfusions (6.6 +/- 4.8 Units vs 3.0 +/- 2.6 Units) besides induction chemotherapy was delayed (60%) and required longer duration of therapy (29.2 +/- 20 vs 6.3 +/- 7.8 days) (P<0.02). Five children (2 ALL, 2 AML, 1 NHL) died but none were infected with B19. INTERPRETATION & CONCLUSIONS: B19 infection should be considered in children with ALL as it frequently caused unexplained anaemia and delay in induction chemotherapy.
机译:背景与目的:白血病和淋巴瘤是感染人类细小病毒B19(B19)的常见儿科血液系统恶性肿瘤。在一些研究中,在维持治疗期间患有急性淋巴细胞白血病(ALL)的儿童中发现贫血,而在淋巴瘤中很少见。我们研究了B19感染的频率及其对儿童新发急性白血病(主要是ALL)和淋巴瘤的影响。方法:收集了35例刚被诊断为血液系统恶性肿瘤(经诱导疗法)的儿童(年龄<12岁,29例男性)的70份血清样本以及34例对照(实体瘤)。对儿童进行临床检查,并通过定量ELISA检测抗B19 IgM抗体,并通过PCR(VP1-VP2)和巢式PCR(VP1 unique)检测B19 DNA。尽可能对组织的病理组织进行检查。结果:在35名儿童中,有22名患有急性白血病,而13名患有淋巴瘤。 35例儿童中有6例(17.1%)出现B19感染(5 ALL,1 NHL),诊断为2例,随访期间为4例,而对照组则没有。在五个B19 IgM阳性ALL(n = 18)儿童中,两个具有B19基因组,两个具有巨大的成原细胞(灯笼细胞;但一个缺少B19 DNA)。在测试的70个血清样本中,八个(11.4%)具有抗B19 IgM,因为两个孩子持续感染B19,一个孩子表现出非典型性斑丘疹(下肢),而十二个孩子(34.3%)具有抗B19 IgG抗体。感染B19的儿童患有无法解释的贫血(80%),需要更多的输血(6.6 +/- 4.8单位vs 3.0 +/- 2.6单位),除了诱导化疗被延迟(60%)并且需要更长的治疗时间(29.2 +/-) 20天vs 6.3 +/- 7.8天)(P <0.02)。 5名儿童(2名ALL,2名AML,1名NHL)死亡,但均未感染B19。结论和结论:ALL患儿应考虑B19感染,因为它经常引起无法解释的贫血和诱导化疗延迟。

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