Genotype-Phenotype Correlation of TNF-α (-238, rs361525) and Cystatin C for Early Detection of Sepsis-Associated AKI and Its Severity in Critically Ill Neonates.

TNF-α (-238, rs361525) 和胱抑素 C 的基因型-表型相关性用于早期检测危重新生儿脓毒症相关 AKI 及其严重程度

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作者:Abdelsattar Shimaa, Al-Amodi Hiba S, Nazih Mahmoud, Salem Eman H M, Mostafa Rasha G, Menshawy Shymaa S, El-Banna Amany A, Abdelgawad Basma M, Nabih Omnia S, Mohsen Yasmin, Abozeid Elaf, Abd El-Hamid Mai El-Sayad, Shoman Nabil A, Ahmed Naglaa Abdelmawgoud, Nabil Mai Mohamed, Mohamed Dalia Abdel-Wahab
Sepsis-associated acute kidney injury (S-AKI) represents a significant health problem associated with adverse outcomes. Our study aimed to assess the value of serum cystatin-C (sCysC) and TNF-α (rs361525) in combination for diagnosing S-AKI patients and predicting their adverse outcomes. The study included 100 critically ill neonates and 100 controls. Patients were categorized into an S-AKI group and a non-AKI group. TNF-α (-238, rs361525) genotyping was performed using RT-PCR, and sCysC was assessed using ELISA. Our study showed a fundamental difference in the genotype frequencies of TNF-α (-238, rs361525) and SNP between S-AKI and non-AKI patients. Furthermore, there was a significant relationship between cystatin C and TNF-α (-238, rs361525), where cystatin C was higher in patients with AA alleles than in patients with GA and GG alleles. Combining GA + AA genotypes with elevated serum cystatin-C levels can serve as a potential diagnostic and prognostic biomarker for AKI development in this population. The GA/AA genotypes independently predicted S-AKI risk (OR = 6.64, p < 0.001). At the same time, elevated sCysC (>9.4 mg/L) emerged as a sensitive biomarker (AUC = 0.848) and independent predictor of adverse outcomes. Collectively, these findings contribute to the growing field of personalized medicine and represent a strategic advantage, enabling prevention-focused care rather than the treatment of established disease.

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