囊性纤维化筛查呈阳性、诊断不确定/与CFTR相关代谢综合征患儿的预后
Outcomes of children with cystic fibrosis screen positive, inconclusive diagnosis/CFTR related metabolic syndrome.
作者信息
Gunnett Mohini A, Baker Elizabeth, Mims Cathy, Self Staci T, Gutierrez Hector H, Guimbellot Jennifer S
机构信息
Department of Pediatrics, Division of Pulmonary and Sleep Medicine, University of Alabama at Birmingham (UAB), Birmingham, AL, United States.
Gregory Fleming James Cystic Fibrosis Research Center, University of Alabama at Birmingham (UAB), Birmingham, AL, United States.
出版信息
Front Pediatr. 2023 Mar 9;11:1127659. doi: 10.3389/fped.2023.1127659. eCollection 2023.
BACKGROUND
Some infants undergoing newborn screening (NBS) tests have inconclusive sweat chloride test (SCT) results that lead to the designation of Cystic Fibrosis Screen Positive, Inconclusive Diagnosis/CFTR-related metabolic syndrome (CFSPID/CRMS). Some proportion of them transition to a CF diagnosis, but no predictive markers can stratify which are at risk for this transition. We report single-center outcomes of children with CRMS.
METHODS
We retrospectively identified all infants born in Alabama from 2008 through 2020 referred to our CF Center with an elevated immunoreactive trypsinogen level (IRT) associated with a cystic fibrosis transmembrane conductance regulator (CFTR) mutation (IRT+/DNA+) who had at least one SCT result documented. Infants were classified per established guidelines as Carrier, CRMS, or CF based on the IRT+/DNA+ and SCT results. The electronic health record was reviewed for follow-up visits until the children received a definitive diagnosis (to carrier or CF) according to current diagnostic guidelines for CF, or through the end of the 2020 year.
RESULTS
Of the 1,346 infants with IRT+ and at least 1 CFTR mutation identified (IRT+/DNA+), 63 (4.7%) were designated as CRMS. Of these infants, 12 (19.1%) transitioned to Carrier status (CRMS-Carrier), 40 (63.5%) of them remained CRMS status (CRMS-Persistent) and 11 (17.5%) of them transitioned to a diagnosis of CF (CRMS-CF). Of the 11 children in the CRMS-CF group, 4 (36%) had an initial SCT 30-39 mmol/L, 4 (36%) had an initial SCT 40-49 mmol/L and 3 (27%) had an initial SCT 50-59 mmol/L. These children also had higher initial sweat tests and greater yearly increases in sweat chloride values than others with CRMS. We found that in comparison to children in the CRMS- group, a greater proportion of children in the CRMS-CF group cultured bacteria like methicillin-resistant had smaller weight-for-height percentiles and remained smaller over time despite slightly greater growth.
CONCLUSION
Infants with an inconclusive diagnosis of CF should continue to receive annual care and management given their potential risk of transition to CF. Further research is needed to assess whether certain phenotypic patterns, clinical symptoms, diagnostic tests or biomarkers could better stratify these children.
背景
一些接受新生儿筛查(NBS)测试的婴儿,其汗液氯化物测试(SCT)结果不明确,导致被判定为囊性纤维化筛查阳性、诊断不确定/与囊性纤维化跨膜传导调节因子(CFTR)相关的代谢综合征(CFSPID/CRMS)。其中一部分人会转变为囊性纤维化(CF)诊断,但没有预测标志物可以区分哪些人有这种转变的风险。我们报告了CRMS患儿的单中心研究结果。
方法
我们回顾性地确定了2008年至2020年在阿拉巴马州出生并被转诊至我们的囊性纤维化中心的所有婴儿,这些婴儿免疫反应性胰蛋白酶原水平(IRT)升高且与囊性纤维化跨膜传导调节因子(CFTR)突变相关(IRT+/DNA+),并且至少有一次记录在案的SCT结果。根据IRT+/DNA+和SCT结果,按照既定指南将婴儿分类为携带者、CRMS或CF。查阅电子健康记录以进行随访,直至儿童根据当前CF诊断指南获得明确诊断(携带者或CF),或直至2020年底。
结果
在1346例IRT+且至少鉴定出1种CFTR突变(IRT+/DNA+)的婴儿中,63例(4.7%)被判定为CRMS。在这些婴儿中,12例(19.1%)转变为携带者状态(CRMS-携带者),40例(63.5%)保持CRMS状态(CRMS-持续),11例(17.5%)转变为CF诊断(CRMS-CF)。在CRMS-CF组的11名儿童中,4例(36%)初始SCT为30-39 mmol/L,4例(36%)初始SCT为40-49 mmol/L,3例(27%)初始SCT为50-59 mmol/L。这些儿童的初始汗液测试值也更高,且汗液氯化物值的年增幅比其他CRMS儿童更大。我们发现,与CRMS-组的儿童相比,CRMS-CF组中培养出耐甲氧西林等细菌的儿童比例更高,身高体重百分位数更小,尽管生长略有增加,但随着时间推移仍保持较小。
结论
CF诊断不确定的婴儿因其有转变为CF的潜在风险,应继续接受年度护理和管理。需要进一步研究以评估某些表型模式、临床症状、诊断测试或生物标志物是否能更好地对这些儿童进行分层。
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