Dose–response relationship between serum N-glycan markers and liver fibrosis in chronic hepatitis B

Author:

Zhang Chi,Liu Yiqi,Wang Lin,Liu Xueen,Chen Cuiying,Zhang Junli,Zhang Chao,Wang Guiqiang,Zhuang Hui,Zhao HongORCID,Cao Li-Hua,Zhang Zhan-Qing,Zhao Wei-Feng,Shang Qing-Hua,Zhang Da-Zhi,Ma An-Lin,Xie Qing,Gui Hong-Lian,Zhang Guo,Liu Ying-Xia,Shang Jia,Xie Shin-Bin,Li Jun,Zhang Xu-Qing,Zou Zhi-Qiang,Chen Yu-Ping,Zhang Zong,Zhang Ming-Xiang,Cheng Jun,Zhang Fu-Chun,Huang Li-Hua,Li Jia-Bin,Meng Qing-Hua,Yu Hai-Bin,Mi Yu-Qiang,Peng Yan-Zhong,Wang Zhi-Jin,Chen Li-Ming,Meng Fan-Ping,Ren Wan-Hua,Bai Lang,Zeng Yi-Lan,Fan Rong,Lou Xian-Zhi,Liang Wei-Feng,

Abstract

Abstract Background Evaluation of liver fibrosis played a monumental role in the diagnosis and monitoring of chronic hepatitis B (CHB). We aimed to explore the value of serum N-glycan markers in liver fibrosis. Methods This multi-center (33 hospitals) study recruited 760 treatment-naïve CHB patients who underwent liver biopsy. Serum N-glycan markers were analyzed by DNA sequencer-assisted fluorophore-assisted with capillary electrophoresis (DSA-FACE) technology. First, we explore the relationship between 12 serum N-glycan markers and the fibrosis stage. Then, we developed a Px score for diagnosing significant fibrosis using the LASSO regression. Next, we compared the diagnostic performances between Px, LSM, APRI, and FIB-4. Finally, we explored the relationships between glycosyltransferase gene and liver fibrosis with RNA-transcriptome sequencing. Results We included 622 CHB participants: male-dominated (69.6%); median age 42.0 (IQR 34.0–50.0); 287 with normal ALT; 73.0% with significant fibrosis. P5(NA2), P8(NA3), and P10(NA4) were opposite to the degree of fibrosis, while other profiles (except for P0[NGA2]) increased with the degree of fibrosis. Seven profiles (P1[NGA2F], P2[NGA2FB], P3[NG1A2F], P4[NG1A2F], P7[NA2FB], P8[NA3], and P9[NA3Fb]) were selected into Px score. Px score was associated with an increased risk of significant fibrosis (for per Px score increase, the risk of significant fibrosis was increased by 3.54 times (OR = 4.54 [2.63–7.82]) in the fully-adjusted generalized linear model. p for trend was <0.001. The diagnostic performance of the Px score was superior to others. Glycosyltransferase genes were overexpressed in liver fibrosis, and glycosylation and glycosyltransferase-related pathways were significantly enriched. Conclusions Serum N-glycan markers were positively correlated with liver fibrosis. Px score had good performance in distinguishing significant fibrosis.

Funder

National Natural Science Foundation of China

China Mega-Project for Infectious Diseases

Publisher

Springer Science and Business Media LLC

Reference30 articles.

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