基于代谢组学的伴慢性肾衰竭牙周炎患者唾液代谢物特征分析

doi:10.3969/j.issn.1674-8115.2026.05.003

上海交通大学学报（医学版） ›› 2026, Vol. 46 ›› Issue (5): 576-584.doi: 10.3969/j.issn.1674-8115.2026.05.003

• 论著 · 基础研究 • 上一篇

基于代谢组学的伴慢性肾衰竭牙周炎患者唾液代谢物特征分析

商迪华¹, 陈慧文¹, 李若琳², 刘英莉², 宋忠臣¹()

^1.上海交通大学医学院附属第九人民医院牙周病科，上海交通大学口腔医学院，国家口腔医学中心，口腔疾病国家临床医学研究中心，上海市口腔医学重点实验室，上海市口腔医学研究所，上海 200011
^2.上海交通大学医学院附属第九人民医院肾脏内科，上海 200011

收稿日期:2025-09-18 接受日期:2025-11-28 出版日期:2026-05-28 发布日期:2026-05-28
通讯作者: 宋忠臣，主任医师，教授，博士；电子信箱：szhongchen@sina.com。
基金资助:
国家自然科学基金(82401195);国家重点研发计划(2023YFC2506300);上海市卫生健康委员会科研项目(20224Y0353);上海交通大学医学院附属第九人民医院临床研究助推计划重点项目(JYLJ202403)

Analysis of salivary metabolite characteristics in periodontitis patients with chronic renal failure based on metabolomics

Shang Dihua¹, Chen Huiwen¹, Li Ruolin², Liu Yingli², Song Zhongchen¹()

^1.Department of Periodontology, Shanghai Ninth People's Hospital, Shanghai Jiao Tong University School of Medicine; College of Stomatology, Shanghai Jiao Tong University; National Center for Stomatology; National Clinical Research Center for Oral Diseases; Shanghai Key Laboratory of Stomatology; Shanghai Research Institute of Stomatology, Shanghai 200011, China
^2.Department of Nephrology, Shanghai Ninth People's Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai 200011, China

Received:2025-09-18 Accepted:2025-11-28 Online:2026-05-28 Published:2026-05-28
Contact: Song Zhongchen, E-mail: szhongchen@sina.com.
Supported by:
National Natural Science Foundation of China(82401195);National Key Research and Development Program of China(2023YFC2506300);Scientific Research Project of Shanghai Municipal Health Commission(20224Y0353);Key Project of Clinical Research Facilitation Program of Shanghai Ninth People′s Hospital, Shanghai Jiao Tong University School of Medicine(JYLJ202403)

摘要/Abstract

摘要：

目的·探讨伴有慢性肾衰竭的牙周炎患者的唾液代谢特征，并分析磷代谢物在其中的作用。方法·纳入在上海交通大学医学院附属第九人民医院肾内科及牙周病科求诊的患者45例，分为牙周炎伴慢性肾衰竭（CRF）组（n=15）、单纯牙周炎（CP）组（n=15）和健康对照（HC）组（n=15）。所有研究对象均接受非刺激性唾液样本的采集和牙周临床检查，记录牙周临床指标以及CRF组患者肾功能指标。采用液相色谱-串联质谱（liquid chromatography-tandem mass spectrometry，LC-MS/MS）技术对唾液样本行非靶向代谢组学检测，通过主成分分析（principal component analysis，PCA）探究组间差异，筛选差异代谢物。通过京都基因与基因组百科全书（Kyoto Encyclopedia of Genes and Genomes，KEGG）数据库对显著差异代谢物进行代谢通路富集分析。选取一个主要差异代谢物，通过体外实验验证该差异代谢物对小鼠胚胎前体成骨细胞MC3T3-E1成骨分化的影响。结果·CRF组的探诊深度、临床附着丧失、牙菌斑指数均显著高于CP组（均P<0.05）。CRF组的尿素（r=0.41）和肌酐水平（r=0.61）与探诊深度均呈正相关，肌酐水平与临床附着丧失（r=0.53）也呈正相关，估算肾小球滤过率（estimated glomerular filtration，eGFR）与探诊深度（r=-0.69）和临床附着丧失（r=-0.56）均呈负相关。PCA结果显示，3组代谢物谱存在显著差异，其中磷酸在3组间差异明显。KEGG分析结果显示，富集的代谢物主要涉及蛋白质消化与吸收、神经活性配体-受体相互作用、鞘脂代谢、坏死性凋亡、癌症中的胆碱代谢、卵巢类固醇生成、鞘脂信号通路与矿物质吸收。体外实验证实，4 mmol/L磷酸盐离子能降低细胞Runt相关转录因子2（Runt-related transcription factor 2，Runx2）、碱性磷酸酶（alkaline phosphatase，Alp）和骨钙素（osteocalcin，Ocn）的mRNA及蛋白表达（均P<0.05），从而抑制MC3T3-E1细胞成骨分化。结论·伴慢性肾衰竭的牙周炎患者牙周组织破坏较单纯牙周炎患者更严重；唾液中磷浓度上调可能是慢性肾脏病加重牙周组织破坏的机制之一；过高的磷浓度可抑制成骨分化。

关键词: 牙周炎, 慢性肾脏病, 唾液代谢组学, 磷, 成骨分化

Abstract:

Objective ·To investigate the salivary metabolic characteristics of periodontitis patients with chronic renal failure (CRF) and analyze the role of phosphorus metabolites in this pathological process. Methods ·A total of 45 patients treated at the Department of Nephrology and the Department of Periodontology, Shanghai Ninth People′s Hospital, Shanghai Jiao Tong University School of Medicine were enrolled, including 15 patients with both periodontitis and CRF in the CRF group, 15 with only periodontitis in the periodontitis (CP) group, and 15 in the healthy control (HC) group. All participants underwent unstimulated saliva collection and periodontal clinical examination. Periodontal clinical parameters were recorded, and renal function indicators of patients in the CRF group were documented. Untargeted metabolomic analysis of saliva samples was performed using liquid chromatography-tandem mass spectrometry (LC-MS/MS). Principal component analysis (PCA) was used to analyze inter-group differences and screen differential metabolites. Significantly differential metabolites were further analyzed for pathway enrichment using the Kyoto Encyclopedia of Genes and Genomes (KEGG) database. One major differential metabolite was selected for in vitro experiments to verify its effect on osteogenic differentiation of mouse embryonic preosteoblasts MC3T3-E1. Results ·Probing depth (PD), clinical attachment loss (CAL), and plaque index (PI) in the CRF group were significantly higher than those in the CP group (all P<0.05). In the CRF group, urea level (r=0.41) and creatinine level (r=0.61) were positively correlated with PD, and creatinine level was also positively correlated with CAL (r=0.53). Estimated glomerular filtration rate (eGFR) was negatively correlated with PD (r=-0.69) and CAL (r=-0.56), respectively. PCA results showed significant differences in metabolite profiles among the three groups, with phosphoric acid presenting remarkable differences. KEGG analysis revealed that the enriched differential metabolites were mainly involved in protein digestion and absorption, neuroactive ligand-receptor interaction, sphingolipid metabolism, necroptosis, choline metabolism in cancer, ovarian steroidogenesis, sphingolipid signaling, and mineral absorption. In vitro experiments confirmed that 4 mmol/L phosphate ions downregulated the mRNA and protein expression levels of Runt-related transcription factor 2 (Runx2), alkaline phosphatase (Alp), and osteocalcin (Ocn) in MC3T3-E1 cells (all P<0.05), thereby inhibiting osteogenic differentiation. Conclusion ·Periodontal tissue destruction is more severe in periodontitis patients complicated with CRF than those without CRF. Upregulated salivary phosphorus concentration may be one of the mechanisms by which chronic kidney disease aggravates periodontal tissue destruction. Excessively high phosphorus concentration can inhibit osteogenic differentiation.

Key words: periodontitis, chronic kidney disease (CKD), salivary metabolomics, phosphorus, osteogenesis

中图分类号:

R781.4

商迪华, 陈慧文, 李若琳, 刘英莉, 宋忠臣. 基于代谢组学的伴慢性肾衰竭牙周炎患者唾液代谢物特征分析[J]. 上海交通大学学报（医学版）, 2026, 46(5): 576-584.

Shang Dihua, Chen Huiwen, Li Ruolin, Liu Yingli, Song Zhongchen. Analysis of salivary metabolite characteristics in periodontitis patients with chronic renal failure based on metabolomics[J]. Journal of Shanghai Jiao Tong University (Medical Science), 2026, 46(5): 576-584.

图/表 7

表1 RT-qPCR引物序列

Tab 1 Primer sequences for RT-qPCR

Gene	Sequence
Gapdh	Forward: 5′-ACAGTCCATGCCATCACTGCC-3′
	Reverse: 5′-GCCTGCTTCACCACCTTCTTG-3′
Runx2	Forward: 5′-CCGGGAATGATGAGAACTA-3′
	Reverse: 5′-ACCGTCCACTGTCACTTT-3′
Alp	Forward: 5′-CCAACTCTTTTGTGCCAGAGA-3′
	Reverse: 5′-GGCTACATTGGTGTTGAGCTTTT-3′
Ocn	Forward: 5′-AAGCAGGAGGGCAATAAGGT-3′
	Reverse: 5′-TTTGTAGGCGGTCTTCAAGC-3′

表2 研究对象的基本特征和牙周临床指标

Tab 2 Basic characteristics and periodontal clinical indicators of all participants

Index	HC group (n=15)	CP group (n=15)	CRF group (n=15)	P value
Age/year	24.43±0.81	51.25±10.88^①	60.69±11.19^②	<0.001
Male/n(%)	8 (53.33)	7 (46.67)	4 (26.67)	0.310
PD/mm	1.73±0.71	3.22±0.86^③	3.57±0.58^④⑤	<0.001
CAL/mm	0	3.13±1.02^⑥	3.74±0.58^⑦⑧	<0.001
PLI	0.71±0.33	1.73±0.26^⑨	1.83±0.18^⑩⑪	<0.001
GI	0.62±0.27	1.75±0.28^⑫	1.78±0.23^⑬	<0.001
BOP/n(%)	45 (8.33)	298 (55.28)^⑭	315 (58.33)^⑮	<0.001

表3 肾功能指标与牙周临床指标相关性

Tab 3 Correlation between renal function indicators and periodontal clinical indicators

Periodontal indicator	Renal function indicator
Periodontal indicator	Urea	Creatinine	eGFR
PD	0.41 (P=0.014)	0.61 (P=0.045)	-0.69 (P=0.001)
CAL	‒	0.53 (P=0.005)	-0.56 (P<0.001)

图1 研究对象唾液样本代谢物组分的PCA结果

Fig 1 PCA result of the metabolite components in saliva samples from the participants

图2 3组唾液差异代谢物的聚类热图

Fig 2 Cluster heatmap of differential salivary metabolites among the 3 groups

图3 KEGG差异代谢通路富集分析

Fig 3 KEGG analysis of enriched differential metabolic pathways

图4 Pi对MC3T3-E1细胞成骨分化的影响Note： A. Effects of different concentrations of Pi on the proliferation activity of MC3T3-E1 cells detected by CCK-8 test. B. ALP staining of MC3T3-E1 cells after 7 d of Pi treatment. C. mRNA expression levels of osteogenic-related factors after 7 d of Pi treatment. D. Protein expression levels of osteogenic-related factors after 7 d of Pi treatment. ①P=0.035, ②P=0.024, ③P=0.007, ④P=0.032, ⑤P=0.006, ⑥P=0.004, ⑦P=0.027, ⑧P=0.042, ⑨P=0.008, ⑩P=0.044, ⑪P=0.007, ⑫P=0.009, ⑬P=0.012, ⑭P=0.025, ⑮P=0.003, ⑯P=0.004, ⑰P=0.017, ⑱P=0.002, ⑲P=0.037, ⑳P=0.048, 21P=0.006. PD—PD173074, an inhibitor of fibroblast growth factor receptor.

Fig 4 Effects of Pi on osteogenic differentiation of MC3T3-E1 cells

参考文献 20

[1]	Bui F Q, Almeida-da-Silva C L C, Huynh B, et al. Association between periodontal pathogens and systemic disease[J]. Biomed J, 2019, 42(1): 27-35.
[2]	Chapple I L C, Hirschfeld J, Cockwell P, et al. Interplay between periodontitis and chronic kidney disease[J]. Nat Rev Nephrol, 2025, 21(4): 226-240.
[3]	Tanaka K, Saito H, Iwasaki T, et al. Association between serum potassium levels and adverse outcomes in chronic kidney disease: the Fukushima CKD cohort study[J]. Clin Exp Nephrol, 2021, 25(4): 410-417.
[4]	Serni L, Caroti L, Barbato L, et al. Association between chronic kidney disease and periodontitis. A systematic review and metanalysis[J]. Oral Dis, 2023, 29(1): 40-50.
[5]	Lertpimonchai A, Rattanasiri S, Tamsailom S, et al. Periodontitis as the risk factor of chronic kidney disease: mediation analysis[J]. J Clin Periodontol, 2019, 46(6): 631-639.
[6]	Miyata Y, Obata Y, Mochizuki Y, et al. Periodontal disease in patients receiving dialysis[J]. Int J Mol Sci, 2019, 20(15): 3805.
[7]	Carvalho J C, Mestrinho H D, Aimée N R, et al. Visible occlusal plaque index predicting caries lesion activity[J]. J Dent Res, 2022, 101(8): 905-911.
[8]	Papapanou P N, Sanz M, Buduneli N, et al. Periodontitis: consensus report of workgroup 2 of the 2017 World Workshop on the Classification of Periodontal and Peri-Implant Diseases and Conditions[J]. J Clin Periodontol, 2018, 45(Suppl 20): S162-S170.
[9]	Wang Y N, Ma S X, Chen Y Y, et al. Chronic kidney disease: biomarker diagnosis to therapeutic targets[J]. Clin Chim Acta, 2019, 499: 54-63.
[10]	Purisinsith S, Kanjanabuch P, Phannajit J, et al. Oral health-related quality of life, a proxy of poor outcomes in patients on peritoneal dialysis[J]. Kidney Int Rep, 2022, 7(10): 2207-2218.
[11]	Troisi J, Belmonte F, Bisogno A, et al. Metabolomic salivary signature of pediatric obesity related liver disease and metabolic syndrome[J]. Nutrients, 2019, 11(2): 274.
[12]	Zhao D, Khawaja A T, Jin L, et al. The directional and non-directional associations of periodontitis with chronic kidney disease: a systematic review and meta-analysis of observational studies[J]. J Periodontal Res, 2018, 53(5): 682-704.
[13]	Maciejczyk M, Szulimowska J, Taranta-Janusz K, et al. Salivary FRAP as a marker of chronic kidney disease progression in children[J]. Antioxidants (Basel), 2019, 8(9): 409.
[14]	Wei Y P, Shi M, Nie Y, et al. Integrated analysis of the salivary microbiome and metabolome in chronic and aggressive periodontitis: a pilot study[J]. Front Microbiol, 2022, 13: 959416.
[15]	Liu F P, Sheng J Y, Hu L, et al. Salivary microbiome in chronic kidney disease: what is its connection to diabetes, hypertension, and immunity?[J]. J Transl Med, 2022, 20(1): 387.
[16]	Chaudhry A, Kassim N K, Zainuddin S L A, et al. Potential effects of non-surgical periodontal therapy on periodontal parameters, inflammatory markers, and kidney function indicators in chronic kidney disease patients with chronic periodontitis[J]. Biomedicines, 2022, 10(11): 2752.
[17]	卢维立, 张旭云, 廖悦, 等. 牙周基础治疗对腹膜透析牙周炎患者临床效果的观察[J]. 上海交通大学学报(医学版), 2020, 40(11): 1489-1494.
	Lu W L, Zhang X Y, Liao Y, et al. Clinical effect of periodontal initial therapy on peritoneal dialysis patients with periodontitis[J]. Journal of Shanghai Jiao Tong University (Medical Science), 2020, 40(11): 1489-1494.
[18]	Sun K, Shen H, Liu Y L, et al. Assessment of alveolar bone and periodontal status in peritoneal dialysis patients[J]. Front Physiol, 2021, 12: 759056.
[19]	Zhang X Y, Chen H W, Lu W L, et al. Characterization of the subgingival microbiota in the peritoneal dialysis patients with periodontitis[J]. Arch Oral Biol, 2020, 115: 104742.
[20]	Raikou V D. Serum phosphate and chronic kidney and cardiovascular disease: phosphorus potential implications in general population[J]. World J Nephrol, 2021, 10(5): 76-87.

基于代谢组学的伴慢性肾衰竭牙周炎患者唾液代谢物特征分析

Analysis of salivary metabolite characteristics in periodontitis patients with chronic renal failure based on metabolomics

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