妊娠合并肝内胆汁淤积症患者胎盘巨噬细胞数量及其亚群变化的临床意义

摘要/Abstract

摘要： 目的分析妊娠合并肝内胆汁淤积症(ICP)患者胎盘巨噬细胞数量及其亚群变化的临床意义。方法选择2022年5月—2024年7月于我院住院治疗并分娩的ICP患者105例,分为轻型ICP组(n=51)和重型ICP组(n=54);同期选择住院正常妊娠健康产妇30名为对照组。比较3组胎盘总巨噬细胞数和M1、M2型巨噬细胞亚群数、IL-10、IL-4、IL-12、INF-γ、TNF-α、TBA、ALT、AST、TBil水平。结果重型ICP组总巨噬细胞、M1型亚群、M2型亚群为(3.04±0.87)%、(19.75±5.73)%、(81.84±10.98)%,轻型ICP组(2.07±0.54)%、(28.42±7.65)%、(72.11±9.86)%,对照组为(0.32±0.10)%、(46.55±12.44)%、(50.76±8.57)%,3组间比较差异有统计学意义(F=171.265、100.055、92.183,均P<0.05)。3组IL-10水平比较无显著差异(P>0.05)。重型ICP组IL-4、IL-12、INF-γ、TNF-α为(37.01±10.35)、(51.44±8.51)、(181.76±15.64)、(108.35±12.73)pg/mL,轻型ICP组(76.33±19.32)、(38.94±7.63)、(153.54±12.65)、(84.53±11.71)pg/mL,对照组为(128.17±22.54)、(23.95±6.42)、(136.22±11.73)、(62.34±10.08)pg/mL,3组间比较差异有统计学意义(F=273.158、122.976、117.775、152.725,均P<0.05)。重型ICP组TBA、AST、ALT、TBil为(83.54±11.35)μmol/L、(198.76±51.85)U/L、(347.95±103.74)U/L、(23.54±3.11)μmol/L,轻型ICP组(30.07±5.23)μmol/L、(50.21±11.38)U/L、(64.35±18.26)U/L、(11.72±2.89)μmol/L,对照组为(14.15±4.57)μmol/L、(28.93±8.76)U/L、(30.17±9.78)U/L、(7.29±1.32)μmol/L,3组间比较差异有统计学意义(F=892.232、349.851、320.673、420.008,均P<0.05)。总巨噬细胞、M2型亚群、IL-4、IL-12、INF-γ、TNF-α水平与ICP患者肝功能均呈正相关(P<0.05);M1型亚群、IL-4水平与ICP患者肝功能均呈负相关(P<0.05);IL-10水平与ICP患者肝功能无显著相关性(P>0.05)。结论 ICP患者胎盘巨噬细胞数量及其亚群分化存在异常,M1/M2型巨噬细胞亚群失衡可能会造成母胎界面免疫微环境损伤,引起发病和病情进展。

关键词: 妊娠合并肝内胆汁淤积症, 胎盘, M1型巨噬细胞, M2型巨噬细胞, 白细胞介素, 肿瘤坏死因子-α, 肝功能

Abstract: Objective To analyze the clinical significance of changes in the number and subpopulations of placental macrophages in patients with intrahepatic cholestasis of pregnancy (ICP). Methods 105 ICP patients who were hospitalized and delivered in our hospital from May 2022 to July 2024 were selected and divided into a mild ICP group (n=51) and a severe ICP group (n=54); during the same period, 30 hospitalized healthy pregnant women were selected as the control group. Compare the total number of placental macrophages and subgroups of M1 and M2 macrophages, as well as the levels of IL-10, IL-4, IL-12, INF - γ, TNF - α, TBA, ALT, AST, and TBil in three groups. Methods The total macrophages, M1 subtype, and M2 subtype in the severe ICP group were (3.04 ± 0.87)%, (19.75 ± 5.73)%, and (81.84 ± 10.98)%, while in the mild ICP group they were (2.07 ± 0.54)%, (28.42 ± 7.65)%, and (72.11 ± 9.86)%. The control group had (0.32 ± 0.10)%, (46.55 ± 12.44)%, and (50.76 ± 8.57)%, respectively. There were statistically significant differences among the three groups (F=171.265, 100.055, 92.183, all P<0.05) There was no significant difference in IL-10 levels among the three groups (P>0.05); The levels of IL-4, IL-12, INF - γ, and TNF - α in the severe ICP group were (37.01 ± 10.35) pg/mL, (51.44 ± 8.51) pg/mL, (181.76 ± 15.64) pg/mL, and (108.35 ± 12.73) pg/mL, while those in the mild ICP group were (76.33 ± 19.32) pg/mL, (38.94 ± 7.63) pg/mL, (153.54 ± 12.65) pg/mL, and (84.53 ± 11.71) pg/mL. The control group had levels of (128.17 ± 22.54) pg/mL, (23.95 ± 6.42) pg/mL, (136.22 ± 11.73) pg/mL, and (62.34 ± 10.08) pg/mL. The differences were statistically significant (F=273.158, 122.976, 117.775, 152.725, all P<0.05). The TBA, AST, ALT, and TBil levels in the heavy ICP group were (83.54 ± 11.35) μmol/L, (198.76 ± 51.85) U/L, (347.95 ± 103.74) U/L, and (23.54 ± 3.11) μmol/L, while those in the light ICP group were (30.07 ± 5.23) μmol/L, (50.21 ± 11.38) U/L, (64.35 ± 18.26) U/L, and (11.72 ± 2.89) μmol/L. The control group had (14.15 ± 4.57) μmol/L, (28.93 ± 8.76) U/L, (30.17 ± 9.78) U/L, and (7.29 ± 1.32) μmol/L. The differences between the three groups were statistically significant (F=892.232, 349.851, 320.673, 420.008, all P<0.05). The levels of total macrophages, M2 subtype, IL-4, IL-12, INF-γ, and TNF-α were positively correlated with liver function in ICP patients (P<0.05); The M1 subtype and IL-4 levels were negatively correlated with liver function in ICP patients (P<0.05); There was no significant correlation between IL-10 levels and liver function in ICP patients (P>0.05). Conclusion There are abnormalities in the number and subpopulation differentiation of placental macrophages in ICP patients. Imbalance of M1/M2 macrophage subpopulations may cause damage to the maternal fetal interface immune microenvironment, resulting in disease onset and progression.

Key words: Pregnancy complicated with intrahepatic cholestasis, Placenta, M1 type macrophages, M2 macrophages, Interleukin, Tumor necrosis factor-α, Liver function

代逃芳, 吴晓容, 曾莉. 妊娠合并肝内胆汁淤积症患者胎盘巨噬细胞数量及其亚群变化的临床意义[J]. 肝脏, 2025, 30(1): 112-116.

DAI Tao-fang, WU Xiao-rong, ZENG Li. Clinical significance of changes in the number and subpopulations of placental macrophages in patients with intrahepatic cholestasis of pregnancy[J]. Chinese Hepatolgy, 2025, 30(1): 112-116.

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