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Causes of death and early life determinants of survival in homozygous sickle cell disease: The Jamaican cohort study from birth

机译:纯合镰状细胞病的死亡原因和生存的早期决定因素:牙买加出生时的队列研究

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摘要

Globally, the majority of persons born with sickle cell disease do not have access to hydroxyurea or more expensive interventions. The objectives were to estimate the survival in homozygous sickle cell disease, unbiased by symptomatic selection and to ascertain the causes of death in a pre-hydroxyurea population. The utility of early life biomarkers and genetically determined phenotypes to predict survival was assessed. A cohort study based on neonatal diagnosis was undertaken at the Sickle Cell Unit, a specialist clinic delivering care to persons with sickle cell disease in Jamaica. Screening of 100,000 deliveries detected 315 babies with homozygous sickle cell disease of whom 311 have been followed from birth for periods up to 43 years. Pneumococcal prophylaxis and teaching mothers splenic palpation were important, inexpensive interventions. Anticipatory guidance, routine care and out-patient acute care were provided. Each participant was classified as alive, dead, or defaulted (usually emigration). Causes of death were ascertained from clinical records and/or post-mortem reports. Survival was assessed using the Kaplan-Meier function. Sex-adjusted Cox semi-parametric proportional hazards and Weibull modelling were used to assess the effects on survival of biomarkers.Survival to 40 years was 55.5% (95% CI 48.7% to 61.7%). Acute Chest Syndrome (n = 31) and septicemia (n = 14) were significant causes of death at all ages. Acute splenic sequestration (n = 12) was the most common cause of early deaths. Survival was significantly shorter in those with lower hemoglobin at 1 year, high total nucleated count at 1 year, and a history of dactylitis ever.In these hydroxyurea naïve patients, survival into midlife was common. Causes of death were often age specific and some may be preventable. Early life biomarkers predictive of decreased survival in SS disease identify a patient group likely to benefit from close clinical supervision and potentially high risk therapies.
机译:在全球范围内,大多数患有镰状细胞疾病的人无法获得羟基脲或更昂贵的干预措施。目的是评估纯合的镰状细胞病的存活率,无症状选择,并确定羟基脲前人群的死亡原因。评估了早期生命生物标志物和遗传确定的表型预测生存的效用。在镰刀病室进行了一项基于新生儿诊断的队列研究,该病专科诊所为牙买加的镰状细胞病患者提供护理。对100,000例分娩的筛查发现315例纯合镰状细胞病婴儿,其中311例从出生起被随访长达43年。预防肺炎球菌和教导母亲脾脏触诊是重要的,廉价的干预措施。提供了预期指导,常规护理和门诊急诊护理。每个参与者都被分类为活着的,死亡的或默认的(通常是移民)。从临床记录和/或验尸报告确定死亡原因。使用Kaplan-Meier函数评估生存率。使用性别调整的Cox半参数比例风险和Weibull建模来评估对生物标志物存活的影响。生存40年的率为55.5%(95%CI为48.7%至61.7%)。各个年龄段的急性胸综合症(n = 31)和败血病(n = 14)都是重要的死亡原因。急性脾隔离症(n = 12)是早期死亡的最常见原因。在1年血红蛋白较低,1年总有核计数高且有过乳腺炎病史的患者中,生存期明显缩短。在这些未接受过羟基脲治疗的患者中,中年生存很常见。死亡原因通常是特定年龄的,有些是可以预防的。可以预测SS疾病存活率降低的早期生物标志物可以确定可能受益于密切的临床监督和潜在的高风险疗法的患者组。

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