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首页> 外文期刊>Journal of clinical laboratory analysis. >Identification and external validation of the optimal FIB‐4 and APRI thresholds for ruling in chronic hepatitis B related liver fibrosis in tertiary care settings
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Identification and external validation of the optimal FIB‐4 and APRI thresholds for ruling in chronic hepatitis B related liver fibrosis in tertiary care settings

机译:鉴定和外部验证最佳FIB-4和慢性乙型肝炎相关肝纤维化术中判定的APRI阈值

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Background With the initially defined thresholds, the most widely used serum biomarkers for staging liver fibrosis (ie, APRI and FIB‐4 scores) proved to be ineffective among patients with chronic hepatitis B virus infection (CHB). Whether optimizing the FIB‐4 and APRI thresholds could improve their diagnostic accuracy requires further research. Methods Using data of treat‐na?ve CHB patients from three tertiary hospitals, we explored the optimal FIB‐4 and APRI thresholds to rule in liver fibrosis accurately. Subsequently, we validated the applicability of the newly defined thresholds to the CHB patients from another two tertiary hospitals. Results The fibrosis stages between discovery cohort (n?=?433) and the external validation cohort (n?=?568) were statistically different ( P ?.001). When ruling in significant fibrosis and advanced fibrosis by the newly defined FIB‐4 thresholds (2.25 and 3.00, respectively), 24.0% and 14.3% of patients, respectively, could be classified with excellent accuracy (PPVs of 91.3% and 80.6%, respectively; misdiagnosis rates of 6.0% and 5.4%, respectively), supported by the internal and external validation tests. Regrettably, the more accurate and robust thresholds of APRI score for ruling in significant fibrosis and advanced fibrosis could not be found. Besides, the FIB‐4 and APRI scores should not be recommended for ruling in cirrhosis because of poor clinical diagnostic performance. Conclusion The newly defined FIB‐4 thresholds for ruling in significant fibrosis and advanced fibrosis showed superior and reproducible clinical diagnostic accuracy. The well‐validated threshold (≥2.25) of FIB‐4 score could aid in antiviral treatment decisions for treat‐na?ve adult CHB patients by accurately ruling in significant fibrosis in tertiary care settings.
机译:背景技术与初始定义的阈值,最广泛使用的血清生物标志物用于分期肝纤维化(即APRI和FIB-4分数)被证明是慢性乙型肝炎病毒感染(CHB)患者的无效。是否优化FIB-4和APRI阈值可以提高其诊断准确性需要进一步的研究。方法使用三个高级医院的治疗 - ve ve患者数据数据,我们探讨了最佳的FIB-4和APRI阈值,准确地统治肝纤维化。随后,我们将新定义的阈值的适用性从另外两位高级医院验证到CHB患者的适用性。结果发现队列(n?=Δ333)和外部验证队之间的纤维化阶段(n?=Δ568)统计学上不同(p <。001)。当通过新定义的FIB-4阈值(分别为22.25和3.00分别为2.25和3.00)分别在显着的纤维化和晚期纤维化,分别为24.0%和14.3%的患者,可以分别归类为优异的精度(PPV分别为91.3%和80.6% ;误诊率分别为6.0%和5.4%),由内部和外部验证测试支持。令人遗憾的是,无法找到在显着纤维化和晚期纤维化中裁决的APRI评分的更准确和强大的阈值。此外,由于临床诊断表现不佳,不应推荐FIB-4和APRI分数在肝硬化中统治。结论新定义的FIB-4用于裁定显着纤维化和晚期纤维化的阈值显示出优异和可重复的临床诊断准确性。验证的阈值(≥2.25)的FIB-4分数可以通过在第三节护理环境中精确地统治在显着的纤维化中来帮助治疗毒性治疗决定。

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