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Clinical Trials and Observations: Biomarkers of splenic function in infants with sickle cell anemia: baseline data from the BABY HUG Trial

机译:临床试验和观察:镰状细胞性贫血婴儿脾功能的生物标志物:BABY HUG试验的基线数据

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摘要

We evaluated spleen function in 193 children with sickle cell anemia 8 to 18 months of age by 99mTc sulfur-colloid liver-spleen scan and correlated results with clinical and laboratory parameters, including 2 splenic biomarkers: pitted cell counts (PIT) and quantitative Howell-Jolly bodies (HJB) enumerated by flow cytometry. Loss of splenic function began before 12 months of age in 86% of infants in association with lower total or fetal hemoglobin and higher white blood cell or reticulocyte counts, reinforcing the need for early diagnosis and diligent preventive care. PIT and HJB correlated well with each other and liver-spleen scan results. Previously described biomarker threshold values did define patients with abnormal splenic function, but our data suggest that normal spleen function is better predicted by PIT of ≤ 1.2% or HJB ≤ 55/106 red blood cells and absent function by PIT ≥ 4.5% or HJB ≥ 665/106. HJB is methodologically advantageous compared with PIT, but both are valid biomarkers of splenic function. This trial was registered at as #.
机译:我们通过 99m Tc硫-胶体肝脾扫描评估了193名8至18个月大的镰状细胞性贫血患儿的脾功能,并将结果与​​临床和实验室参数相关联,包括2种脾脏生物标志物:凹孔细胞计数(PIT)和通过流式细胞仪计数的定量霍威尔-乔利体(HJB)。 86%的婴儿因总血红蛋白或胎儿血红蛋白降低以及白细胞或网织红细胞计数升高而在12个月前开始脾功能丧失,这增加了对早期诊断和勤奋的预防保健的需求。 PIT和HJB彼此之间以及肝脾扫描结果之间的相关性很好。先前描述的生物标志物阈值确实定义了脾功能异常的患者,但我们的数据表明,PIT≤1.2%或HJB≤55/10 6 红细胞和功能缺失可更好地预测脾功能正常PIT≥4.5%或HJB≥665/10 6 。与PIT相比,HJB在方法上具有优势,但两者都是脾功能的有效生物标志物。该试用版注册为#。

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