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首页> 外文期刊>Bone marrow transplantation >Screening for cytomegalovirus (CMV) infection in allogeneic bone marrow transplantation using a quantitative whole blood polymerase chain reaction (PCR) method: analysis of potential risk factors for CMV infection.
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Screening for cytomegalovirus (CMV) infection in allogeneic bone marrow transplantation using a quantitative whole blood polymerase chain reaction (PCR) method: analysis of potential risk factors for CMV infection.

机译:使用定量全血聚合酶链反应(PCR)方法筛选同种异体骨髓移植中的巨细胞病毒(CMV)感染:分析CMV感染的潜在危险因素。

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Potential risk factors for CMV infection and the use of quantitative CMV PCR screening to guide pre-emptive anti-CMV therapy were reviewed retrospectively in 32 allogeneic bone marrow transplant patients accrued over a 2-year period. Significant CMV PCR positivity (an indicator of CMV infection) developed in 34% of patients. When analysed by recipient CMV IgG serostatus, 69% of seropositive recipients developed significant CMV PCR positivity while none of the seronegative recipients did so (P = 0.00007). Considering only the seropositive recipients, 100% of those who received the low intensity campath-1H/fludarabine/melphalan 'mini-allograft' conditioning regimen developed significant CMV PCR positivity, while only 44% of those who had received cyclophosphamide/TBI did so (P = 0.0337). The mean time to first episode of significant CMV PCR positivity for those who had received campath/fludarabine/melphalan was 25 days while for those who had received cyclophosphamide/TBI, this was 66 days (P = 0.0372). For the first episode of significant CMV PCR positivity, the mean index and peak CMV PCR counts for those who had received campath/fludarabine/melphalan were 4.54 and 5.22 log copies/ml respectively, while for cyclophosphamide/TBI, the corresponding figures were 3.85 and 4.12 log copies/ml respectively (P = 0.2986 and P = 0.0472 for index and peak values). 85% of those who had significant CMV PCR positivity with the campath/fludarabine/melphalan regimen developed more than one such episode, while 50% of those receiving cyclophosphamide/TBI regimen did so (P = 0.491). Significant CMV PCR positivity was associated with symptoms in a proportion of patients (pyrexia 45%, cough 18%, rise in AST 72%). No patient developed overt CMV disease. CMV PCR is useful for guiding pre-emptive anti-CMV therapy and for monitoring response.
机译:回顾性地回顾了两年内累积的32名同种异体骨髓移植患者中CMV感染的潜在危险因素以及定量CMV PCR筛选指导先发性抗CMV治疗的应用。 34%的患者出现了显着的CMV PCR阳性(CMV感染的指标)。通过接受者CMV IgG血清状态分析时,有69%的血清反应阳性接受者表现出显着的CMV PCR阳性,而血清阴性接受者则没有(P = 0.00007)。仅考虑血清反应阳性的接受者,接受低强度campath-1H /氟达拉滨/美法仑“微型同种异体移植”治疗方案的接受者中,有100%表现出显着的CMV PCR阳性,而接受环磷酰胺/ TBI的接受者只有44%( P = 0.0337)。接受Campath / fludarabine / melphalan的患者第一次出现CMV PCR阳性的平均时间为25天,而接受环磷酰胺/ TBI的患者则为66天(P = 0.0372)。对于首例显着的CMV PCR阳性,接受坎普/氟达拉滨/美法仑的人的平均指数和CMV PCR峰值分别为4.54和5.22 log拷贝/ ml,而环磷酰胺/ TBI的相应指数为3.85和5。分别为4.12对数拷贝/ ml(对于指数和峰值,P = 0.2986和P = 0.0472)。在采用campath / fludarabine / melphalan方案具有显着CMV PCR阳性的患者中,有85%发生了多于一种这样的发作,而接受环磷酰胺/ TBI方案的患者中有50%发生了这种情况(P = 0.491)。显着的CMV PCR阳性与一部分患者的症状相关(发热45%,咳嗽18%,AST升高72%)。没有患者出现明显的CMV疾病。 CMV PCR可用于指导先发性抗CMV治疗和监测反应。

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