Significant roles of anti-aging protein klotho and fibroblast growth factor23 in cardiovascular disease

The klotho gene has been identified as an aging suppressor that encodes a protein involved in cardiovascular disease （CVD）. The inac- tivation of the klotho gene causes serious systemic disorders resembling human aging, such as atherosderosis, diffuse vascular calcification and shortened life span. Klotho has been demonstrated to ameliorate vascular endothelial dysfunction and delay vascular calcification. Fur- thermore, klotho gene polymorphisms in the human are associated with various cardiovascular events. Recent experiments show that klotho may reduce transient receptor potential canonical6 （TRPC6） channels, resulting in protecting the heart from hypertrophy and systolic dys- function. Fibroblast growth factor23 （FGF23） is a bone-derived hormone that plays an important role in the regulation of phosphate and vi- tamin D metabolism. FGF23 accelerates urinary phosphate excretion and suppresses 1,25-dihydroxy vitaminD3 （1,25（OH）2D3）synthesis in the presence ofFGF receptorl （FGFR1） and its co-receptor ldotho, principally in the kidney. The hormonal affects of circulating klotho pro- tein and FGF23 on vascular and heart have contributed to an understanding of their roles in the pathophysiology of arterial stiffness and left ventricular hypertrophy. Klotho and FGF23 appear to play a critical role in the pathogenesis of vascular disease, and may represent a novel potential therapeutic strategy for clinical intervention.

The hypoxia-inducible factor-1α activates ectopic production of fibroblast growth factor 23 in tumor-induced osteomalacia

Tumor-induced osteomalacia （TIO） is a rare paraneoplastic syndrome in which ectopic production of fibroblast growth factor 23 （FGF23） by non-malignant mesenchymal tumors causes phosphate wasting and bone fractures. Recent studies have implicated the hypoxia-inducible factor-la （HIF-la） in other phosphate wasting disorders caused by elevated FGF23, including X-linked hypophosphatemic rickets and autosomal dominant hypophosphatemia. Here we provide evidence that HIF-la mediates aberrant FGF23 in TIO by transcriptionally activating its promoter. Immunohistochemical studies in phosphaturic mesenchymal tumors resected from patients with documented TIO showed that HIF-la and FGF23 were co-localized in spindle- shaped cells adjacent to blood vessels. Cultured tumor tissue produced high levels of intact FGF23 and demonstrated increased expression of HIF-la protein. Transfection of MC3T3-E1 and Saos-2 cells with a HIF-la expression construct induced the activity of a FGF23 reporter construct. Prior treatment of tumor organ cultures with HIF-la inhibitors decreased HIF-la and FGF23 protein accumulation and inhibited HIF-la-induced luciferase reporter activity in transfected cells. Chromatin immunoprecipitation assays confirmed binding to a HIF-la consensus sequence within the proximal FGF23 promoter, which was eliminated by treatment with a HIF-la inhibitor. These results show for the first time that HIF-la is a direct transcriptional activator of FGF23 and suggest that upregulation of HIF-la activity in TIO contributes to the aberrant FGF23 production in these patients.

Fibroblast growth factor 23 and bone mineralisation

Fibroblast growth factor 23 （FGF23） is a hormone that is mainly secreted by osteocytes and osteoblasts in bone. The critical role of FGF23 in mineral ion homeostasis was first identified in human genetic and acquired rachitic diseases and has been further characterised in animal models. Recent studies have revealed that the levels of FGF23 increase significantly at the very early stages of chronic kidney disease （CKD） and may play a critical role in mineral ion disorders and bone metabolism in these patients. Our recent publications have also shown that FGF23 and its cofactor, Klotho, may play an independent role in directly regulating bone mineralisation instead of producing a systematic effect. In this review, we will discuss the new role of FGF23 in bone mineralisation and the pathophysiology of CKD-related bone disorders.

Tumor-induced osteomalacia with elevated fibroblast growth factor 23: a case of phosphaturic mesenchymal tumor mixed with connective tissue variants and review of the literature

Tumor-induced osteomalacia (TIO), or oncogenic osteomalacia (OOM), is a rare acquired paraneoplastic disease characterized by renal phosphate wasting and hypophosphatemia. Recent evidence shows that tumor-overexpressed fibroblast growth factor 23 (FGF23) is responsible for the hypophosphatemia and osteomalacia. The tumors associated with TIO are usually phosphaturic mesenchymal tumor mixed connective tissue variants (PMTMCT). Surgical removal of the responsible tumors is clinically essential for the treatment of TIO. However, identifying the responsible tumors is often difficult. Here, we report a case of a TIO patient with elevated serum FGF23 levels suffering from bone pain and hypophosphatemia for more than three years. A tumor was finally located in first metacarpal bone by octreotide scintigraphy and she was cured by surgery. After complete excision of the tumor, serum FGF23 levels rapidly decreased, dropping to 54.7% of the preoperative level one hour after surgery and eventually to a little below normal. The patient's serum phosphate level rapidly improved and returned to normal level in four days. Accordingly, her clinical symptoms were greatly improved within one month after surgery. There was no sign of tumor recurrence during an 18-month period of follow-up. According to pathology, the tumor was originally diagnosed as "glomangioma" based upon a biopsy sample, "proliferative giant cell tumor of tendon sheath" based upon sections of tumor, and finally diagnosed as PMTMCT by consultation one year after surgery. In conclusion, although an extremely rare disease, clinicians and pathologists should be aware of the existence of TIO and PMTMCT, respectively.

Significance of serum fibroblast growth factor-23 and miR-208b in pathogenesis of atrial fibrillation and their relationship with prognosis

BACKGROUND The incidence and prevalence of atrial fibrillation are increasing each year,and this condition is one of the most common clinical arrhythmias.AIM To investigate the levels and significance of serum fibroblast growth factor 23(FGF-23)and miR-208 b in patients with atrial fibrillation and their relationship with prognosis.METHODS From May 2018 to October 2019,240 patients with atrial fibrillation were selected as an observation group,including 134 with paroxysmal atrial fibrillation and 106 with persistent atrial fibrillation;150 patients with healthy sinus rhythm were selected as a control group.The serum levels of FGF-23 and miR-208 b in the two groups were measured.In the observation group,cardiac parameters were determined by echocardiography.RESULTS The serum levels of FGF-23 and miR-208 b in the observation group were 210.20±89.60 ng/mL and 5.30±1.22 ng/mL,which were significantly higher than the corresponding values in the control group(P<0.05).In the observation group,the serum levels of FGF-23 and miR-208 b in patients with persistent atrial fibrillation were 234.22±70.05 ng/mL and 5.83±1.00 ng/mL,which were significantly higher than the corresponding values in patients with paroxysmal atrial fibrillation(P<0.05).The left atrial dimension(LAD)of patients with persistent atrial fibrillation was 38.81±5.11 mm,which was significantly higher than that of patients with paroxysmal atrial fibrillation(P>0.05).The serum levels of FGF-23and miR-208 b were positively correlated with the LAD(r=0.411 and 0.382,P<0.05).In the observation group,the serum levels of FGF-23 and miR-208 b in patients with a major cardiovascular event(MACE)were 243.30±72.29 ng/mL and 6.12±1.12 ng/mL,which were significantly higher than the corresponding values in patients without a MACE(P<0.05).CONCLUSION The serum levels of FGF-23 and miR-208 b are increased in patients with atrial fibrillation and are related to the type of disease,cardiac parameters,and prognosis.

Fibroblast Growth Factor 23 and Left Ventricular Hypertrophy in Hemodialysis Patients

Background: Left ventricular hypertrophy (LVH) is a common cardiovascular complication and an independent risk factor for cardiovascular death in hemodialysis (HD) patients. Previous studies have shown that fibroblast growth factor 23 (FGF23), which has an important role in phosphate metabolism, is elevated in HD patients. Objectives: The aim of this study was to determine the association of FGF23 and LVH and the prognostic value of serum FGF23 level in HD patients. One hundred seven HD patients were evaluated for LVH by echocardiography. Serum FGF23 levels were measured using a commercial enzyme-linked immunosorbent assay kit. Results: Patients with LVH were more likely to have higher systolic blood pressure (BP) and LVH was significantly associated with female gender and higher serum levels of phosphate and calcium ×phosphate products. LVH was also associated with higher serum FGF23 level. Multivariate analysis indicated that serum FGF23 level, systolic BP, and serum phosphate level remained correlated with LVH. This suggested that serum FGF23 level is independently associated with LVH in our HD patients. Cox analysis indicated no significant difference in risk of death for patients with elevated serum FGF23 level. Conclusion: LVH has a high prevalence in HD patients, and FGF23 is independently associated with LVH but is not a predictor for prognosis during a 4-year follow-up period.

狼疮性肾炎患者血清FGF-23、Gas6水平与疾病活动性的关系

目的探讨狼疮性肾炎(LN)患者血清成纤维细胞生长因子23(FGF-23)、生长停滞特异性蛋白6(Gas6)水平与疾病活动性的关系。方法选择2021年3月—2024年3月延安市人民医院风湿免疫科收治的LN患者119例为LN组,并根据系统性红斑狼疮疾病活动指数2000(SLEDAI-2000)评分分为活动亚组70例和非活动亚组49例,另选取同期医院健康体检者105例为健康对照组。采用酶联免疫吸附试验检测血清FGF-23、Gas6水平;Pearson相关分析血清FGF-23、Gas6水平与肾功能指标、SLEDAI-2000评分的相关性;多因素Logistic回归分析LN患者疾病活动性的影响因素;受试者工作特征(ROC)曲线评价血清FGF-23、Gas6水平对LN患者疾病活动性的诊断价值。结果LN组血清FGF-23、Gas6水平均高于健康对照组(t/P=21.040/<0.001、7.389/<0.001);活动亚组收缩压、舒张压、尿素氮(BUN)、血肌酐(SCr)、尿蛋白、SLEDAI-2000评分、FGF-23、Gas6均高于非活动亚组(t/P=2.356/0.020、3.717/<0.001、11.867/<0.001、17.152/<0.001、30.579/<0.001、19.439/<0.001、11.284/<0.001、10.818/<0.001),补体C3、C4水平低于非活动亚组(t/P=6.233/<0.001、12.329/<0.001);血清FGF-23、Gas6水平分别与BUN、SCr、尿蛋白、SLEDAI-2000评分呈正相关(FGF-23:r/P=0.410/<0.001、0.395/<0.001、0.326/0.002、0.563/<0.001;Gas6:r/P=0.352/<0.001、0.384/<0.001、0.311/0.008、0.509/<0.001),与补体C3、C4水平呈负相关(FGF-23:r/P=-0.408/<0.001、-0.377/<0.001;Gas6:r/P=-0.376/<0.001、-0.321/<0.001);多因素Logistic回归分析显示,高FGF-23、Gas6、尿蛋白水平是LN患者疾病活动的独立危险因素[OR(95%CI)=2.136(1.224~3.727)、1.865(1.171~2.967)、2.539(1.416~4.554)];血清FGF-23、Gas6水平及二者联合诊断LN患者疾病活动性的曲线下面积(AUC)分别为0.804、0.834、0.938,二者联合的AUC大于各自单独诊断(Z/P=3.843/<0.001、3.270/<0.001)。结论LN患者血清FGF-23、Gas6水平均增高,且与LN肾功能损伤、补体水平降低及疾病活动性增加有关。联合检测FGF-23、Gas6可有效鉴别LN疾病活动性。

血清ANGPTL3、FGF-23水平与急性脑梗死患者病情严重程度及预后的关系

目的探讨血清血管生成素样蛋白3(ANGPTL3)、成纤维细胞生长因子-23(FGF-23)水平与急性脑梗死(ACI)患者病情严重程度及预后的关系。方法选取2022年3月至2023年2月该院收治的102例ACI患者为ACI组,根据脑梗死体积分为小梗死组、中梗死组和大梗死组,根据美国国立卫生研究院卒中量表(NIHSS)评分分为轻度损伤组、中度损伤组和重度损伤组,根据随访90 d后患者预后情况[改良Rankin量表(mRS)评分]分为预后良好组和预后不良组。另招募同期在该院体检的100例健康者作为对照组。采用酶联免疫吸附试验检测血清ANGPTL3、FGF-23水平。绘制受试者工作特征(ROC)曲线分析血清ANGPTL3、FGF-23对ACI患者预后不良的预测价值。采用Pearson相关分析血清ANGPTL3、FGF-23水平与NIHSS评分及mRS评分的相关性,采用Spearman相关分析血清ANGPTL3、FGF-23水平与脑梗死体积的相关性。结果ACI组血清ANGPTL3、FGF-23水平显著高于对照组(P<0.05)。根据脑梗死体积将ACI患者分为小梗死组29例,中梗死组46例,大梗死组27例;大梗死组血清ANGPTL3、FGF-23水平显著高于小梗死组、中梗死组(P<0.05),中梗死组血清ANGPTL3、FGF-23水平显著高于小梗死组(P<0.05)。根据NIHSS评分将ACI患者分为轻度损伤组41例,中度损伤组38例,重度损伤组23例;重度损伤组血清ANGPTL3、FGF-23水平显著高于轻度损伤组、中度损伤组(P<0.05),中度损伤组血清ANGPTL3、FGF-23水平高于轻度损伤组(P<0.05)。根据随访结果将ACI患者分为预后良好组68例,预后不良组34例;预后不良组血清ANGPTL3、FGF-23水平显著高于预后良好组(P<0.05)。ROC曲线分析结果显示,血清ANGPTL3、FGF-23单独及联合预测ACI患者预后不良的曲线下面积(AUC)分别为0.795、0.856、0.923,灵敏度分别为70.59%、67.65%、88.24%,特异度分别为83.82%、91.18%、82.59%,且二者联合预测ACI患者预后不良的AUC显著高于各项指标单独预测(ZANGPTL3=3.232,P<0.05;Z_(FGF)-23=2.216,P<0.05)。相关性分析结果显示,ACI患者血清ANGPTL3、FGF-23水平与NIHSS评分、脑梗死体积及mRS评分均呈正相关(P<0.05)。结论ACI患者血清ANGPTL3、FGF-23水平上升,且与梗死体积、神经功能缺损严重程度和预后相关,二者联合检测可有效预测ACI预后情况。

血清CERP、SF、α-Klotho、FGF-23水平在2型糖尿病患者白蛋白尿进展中的预测价值

目的分析血清铜蓝蛋白(ceruloplasmin,CERP)、血清铁蛋白(serum ferritin,SF)、α-Klotho、成纤维细胞生长因子-23(fibroblast growth factor,FGF-23)在2型糖尿病患者白蛋白尿进展中的预测价值。方法选择2020年6月至2022年5月沭阳医院内分泌科因控制血糖重复收住院的120例2型糖尿病患者进行回顾性队列研究,将首次住院和第二次住院的资料分别作为基线资料和随访资料。根据基线中患者白蛋白尿情况将其分为3组:无白蛋白尿组、微量白蛋白尿组、大量白蛋白尿组,比较3组患者中CERP、SF、α-Klotho、FGF-23水平的差异;根据随访资料评价白蛋白尿进展的情况,比较白蛋白尿进展的患者与未进展的患者的基线临床资料及其CERP、SF、α-Klotho、FGF-23水平的差异,采用logistic回归分析白蛋白尿进展的影响因素,采用ROC曲线分析白蛋白尿进展的预测指标。结果随着2型糖尿病患者尿白蛋白水平升高,血清CERP、SF、FGF-23水平升高,而α-Klotho水平降低(P<0.05);白蛋白尿进展的2型糖尿病患者的糖尿病病程长于未进展的2型糖尿病患者,其二甲双胍及SGLT2抑制剂(SGLT2i)使用比例、α-Klotho水平均低于未进展的2型糖尿病患者,其高血压比例、FBG、UA、CERP、SF、FGF-23水平均高于未进展的2型糖尿病患者,差异有统计学意义(P<0.05);logistic回归分析显示CERP、SF、FGF-23水平升高是白蛋白尿进展的危险因素,而使用二甲双胍及SGLT2i以及α-Klotho水平的升高均是白蛋白尿进展的保护因素;ROC曲线分析显示首次住院时血清CERP、SF、α-Klotho、FGF-23的水平对白蛋白尿进展具有预测价值,logistic回归方程的联合指标预测尿白蛋白的灵敏度和特异性均优于单一指标。结论血清CERP、SF、FGF-23水平的升高及α-Klotho水平的降低与2型糖尿病患者中白蛋白尿进展有关,检测4项血清指标对白蛋白尿进展具有预测价值。

血清FGF-23、PLGF、TyG指数联合检测对妊娠期糖尿病患者不良妊娠结局的预测效能

目的:探讨血清成纤维细胞生长因子-23(Fibroblast growth factor-23,FGF-23)、胎盘生长因子(Placenta growth factor,PLGF)、甘油三酯葡萄糖(Triglyceride glucoseindex,TyG)指数联合检测对妊娠期糖尿病(Gestational diabetes mellitus,GDM)患者不良妊娠结局的预测价值。方法:选取2020年2月-2022年12月在夏邑县中心医院妇产科产检的132例GDM患者为GDM组,并选择同期132例正常孕妇作为对照组。GDM组患者根据妊娠结局不同分为良好妊娠结局和不良妊娠结局亚组,比较GDM组和对照组及不同妊娠结局GDM患者血清FGF-23、PLGF水平及TyG指数,分析血清FGF-23、PLGF、TyG指数联合检测对GDM患者妊娠结局的预测效能。结果:GDM组血清FGF-23水平及TyG指数高于对照组,血清PLGF水平低于对照组(P<0.05),GDM组发生不良妊娠结局50例,不良妊娠结局发生率为37.88%;不良妊娠结局患者血清FGF-23水平及TyG指数高于良好妊娠结局,血清PLGF水平低于良好妊娠结局(P<0.05),血清FGF-23、PLGF、TyG指数联合检测预测GDM患者不良妊娠结局的AUC、特异度、敏感度分别为0.835、87.12%、86.36%,均高于血清FGF-23、PLGF、TyG指数单独预测指标(P<0.001)。结论:GDF患者的血清FGF-23水平、TyG指数较高,血清PLGF水平较低。血清FGF-23、PLGF水平、TyG指数联合检测对GDF患者的不良妊娠结局有较高的预测价值,临床可根据GDF患者血清FGF-23、PLGF水平及TyG指数,及早进行干预,以减少GDM不良妊娠结局的发生,保障母婴健康。

血清Hcy及FGF-23预测血液透析治疗尿毒症合并高血压患者并发心脑血管事件的价值

目的分析血清同型半胱氨酸(Hcy)、成纤维细胞生长因子-23(FGF-23)预测血液透析治疗尿毒症合并高血压患者并发心脑血管事件的价值。方法回顾性分析,选取2019年2月至2022年12月在黄石市中医医院收治的98例行血液透析治疗的尿毒症合并高血压患者的临床资料,其中男58例、女40例,年龄53~76(64.18±5.39)岁;另收集患者血清Hcy、FGF-23等临床资料,随访1年。统计随访期间患者发生心脑血管事件情况,采用t检验、χ^(2)检验及logistic回归分析影响血液透析治疗尿毒症合并高血压患者心脑血管事件发生的因素,并绘制受试者操作特征曲线(ROC)分析Hcy与FGF-23预测其发生心脑血管事件的价值。结果98例行血液透析治疗的尿毒症合并高血压患者中,有37例(37.76%)出现心脑血管事件,其余61例(62.24%)未出现心脑血管事件。两组患者性别、年龄、体质量指数、吸烟史、饮酒史、心率、高血压病程、收缩压、舒张压、降压药物使用种类、空腹血糖、三酰甘油、总胆固醇、高密度脂蛋白胆固醇、前白蛋白、转铁蛋白、尿素氮、肌酐、尿酸、血清丙氨酸转氨酶、γ-谷氨酰转移酶、血钙、血磷、总尿素清除指数、血甲状旁腺素、左室射血分数比较,差异均无统计学意义(均P>0.05);心脑血管事件组透析龄、血白蛋白、低密度脂蛋白胆固醇、尿白蛋白排泄率、红细胞分布宽度、Hcy、FGF-23均高于非心脑血管事件组[(4.83±0.81)年比(4.39±0.58)年、(36.33±5.08)g/L比(32.66±5.39)g/L、(3.59±0.75)mmol/L比(3.25±0.35)mmol/L、(38.77±4.43)mg/24 h比(35.54±4.41)mg/24 h、(15.59±2.19)%比(13.21±1.16)%、(18.82±2.31)μmol/L比(14.46±2.20)μmol/L、(189.71±32.69)ng/L比(154.59±27.68)ng/L],估算肾小球滤过率(eGFR)低于非心脑血管事件组[(40.56±7.12)ml/min/1.73m2比(46.37±6.23)ml/min/1.73 m2],差异均有统计学意义(t=3.126、3.388、3.043、3.509、7.303、9.333、5.683、4.239,均P<0.05)。logistic多因素回归分析显示,透析龄、Hcy、FGF-23、eGFR水平是影响血液透析治疗尿毒症合并高血压患者心脑血管事件发生的因素(均P<0.05)。ROC分析结果显示,Hcy、FGF-23及二者联合预测血液透析治疗尿毒症合并高血压患者发生心脑血管事件的灵敏度分别为71.68%、76.57%、78.04%,特异度分别为78.59%、74.31%、89.36%,曲线下面积(AUC)分别为0.768、0.745、0.886。结论血清Hcy、FGF-23水平与血液透析治疗尿毒症合并高血压患者并发心脑血管事件有关,Hcy、FGF-23处于高水平时心脑血管事件发生风险更高,二者联合预测血液透析治疗尿毒症合并高血压患者并发心脑血管事件效能较高。

血清Sclerostin、miR-155-5p、FGF-23水平联合检测对尿毒症血液透析患者发生血管钙化的诊断价值

目的:探讨尿毒症血液透析患者血清骨硬化蛋白(Sclerostin,Sost)、微小RNA-155-5p(microRNA-155-5p,miR-155-5p)、成纤维细胞生长因子-23(Fibroblast growth factor-23,FGF-23)水平,分析其对血管钙化的诊断价值。方法:选取2020年1月~2022年12月本院收治的92例尿毒症血液透析患者作为研究对象,依据是否发生血管钙化分为钙化组(n=68)和非钙化组(n=24)。检测并比较两组生化指标及血清Sost、miR-155-5p、FGF-23水平。分析血清指标与生化指标、钙化程度相关性。采用受试者工作特征曲线(Receiver operating characteristic curve,ROC)分析血清指标对血管钙化的诊断价值。结果:钙化组血清Sost、miR-155-5p、FGF-23水平高于非钙化组(P<0.05);血清Sost、miR-155-5p、FGF-23水平与骨形成蛋白2(Bone morphogenetic protein 2,BMP-2)、全段甲状旁腺激素(Intact parathyroid hormone,iPTH)、钙化程度呈正相关(P<0.05);血清Sost、miR-155-5p、FGF-23联合诊断血管钙化的AUC大于单项指标诊断(P<0.05)。结论:尿毒症血液透析患者中,血管钙化者血清Sost、miR-155-5p、FGF-23水平升高,且与血管钙化程度呈正相关,联合检测其水平对血管钙化具有一定诊断价值。

血清脂联素、成纤维生长因子-23在心脏瓣膜置换术患者预后中的评估价值

目的探讨血清脂联素、成纤维生长因子-23(FGF23)水平在心脏瓣膜置换术患者预后中的评估价值。方法选取行心脏瓣膜置换术的患者98例为研究组。根据研究组患者的预后情况分为预后良好组(n=67)和预后不良组(n=31)。选取同期健康体检者90例为对照组。采用Spearman法分析血清脂联素、FGF23水平分别与血浆N末端B型利钠肽前体(NT-proBNP)水平和急性生理学与慢性健康状况评分系统Ⅱ(APACHEⅡ)评分的相关性。采用多因素Logistic回归分析法分析心脏瓣膜置换术患者预后的影响因素。绘制受试者工作特征(ROC)曲线分析血清脂联素、FGF23水平对心脏瓣膜置换术患者预后的预测价值。结果研究组血清FGF23、NT-proBNP水平、APACHEⅡ评分高于对照组,血清脂联素水平低于对照组,差异有统计学意义(P<0.05)。预后不良组血清FGF23、NT-proBNP水平和APACHEⅡ评分高于预后良好组,血清脂联素水平低于预后良好组,差异有统计学意义(P<0.05)。患者的血清FGF23水平与NT-proBNP水平、APACHEⅡ评分呈正相关(P<0.05)。血清脂联素水平与NT-proBNP水平、APACHEⅡ评分呈负相关(P<0.05)。血清脂联素、FGF23、NT-proBNP水平和APACHEⅡ评分为心脏瓣膜置换术患者预后的影响因素(P<0.05)。血清脂联素、FGF23单独预测和联合预测心脏瓣膜置换术患者预后的曲线下面积(AUC)分别为0.862、0.807、0.911。脂联素、FGF23联合预测的AUC大于单独预测,差异有统计学意义(P<0.05)。结论血清脂联素、FGF23联合预测心脏瓣膜置换术患者预后的效果较好。血清脂联素、FGF23有望成为评估心脏瓣膜置换术患者预后效果的有效指标。

血清FGF-23与维持性血液透析患者透中低血压发生的关系

目的:探讨维持性血液透析(maintenance hemodialysis,MHD)患者发生透中低血压(intradialytic hypotension,IDH)与血清中可溶性klotho(soluble klotho,sKl)和成纤维细胞生长因子23(fibroblast growth factor23,FGF23)之间的关系。方法:横断面收集MHD患者病情资料,根据最近1个月内透析记录,将MHD患者分成无透中低血压组(N-IDH)和透析中低血压组(IDH)。收集患者同期实验室检查结果,并采集患者血清样本,检测血清FGF23与sKl水平。比较N-IDH与IDH患者之间生化指标差异。结果:共收集临床信息完整及血清标本完整患者80例,其中IDH发生率为77.5%,独立样本t检验分析结果提示五个指标在N-IDH和IDH组之间差异存在统计学意义,血铁蛋白(P=0.046)、血三酰甘油(P=0.045)、血iPTH(P=0.047)、钙磷乘积(P=0.042)和血清FGF23(P<0.001)。而sKl在两组间差异无统计学意义(P=0.747)。相关性检验提示IDH组的患者IDH发生频率与血清FGF23浓度的相关关系分析显示两者呈正相关(r=0.722,P<0.001)。结论:本组病例提示血清FGF23的水平与MHD患者透析中低血压的发生密切相关。

维持性血液透析患者外周血FGF-23水平与血管钙化相关性研究

目的:了解维持性血液透析患者的外周血成纤维细胞生长因子(FGF-23)水平和血管钙化情况,探讨两者的相关性。方法:收集90例维持性血液透析患者的临床资料,通过X线平片评价血管钙化情况,双抗体夹心ABC-ELISA法测定外周血FGF-23水平,Spearman相关分析血管钙化评分与FGF-23水平的相关性,多元Logistic回归分析血管钙化的危险因素。结果:血管钙化评分≥3分患者的外周血FGF-23水平显著高于钙化评分<3分患者,(98.21±13.55)VS(58.65±6.36)pg/ml,P<0.05。Spearman秩相关显示血FGF-23水平与血管中重度钙化存在相关(r=0.315),并且FGF-23水平越高,血管钙化程度越重(r=0.328),P<0.05。多元Logistic回归分析结果显示,FGF-23浓度是血液透析患者中小动脉钙化的独立危险因素。结论:维持性血液透析患者普遍存在的血管钙化与血浆FGF-23水平相关,FGF-23水平是除老龄、糖尿病、残余肾功能丧失等传统因素之外的血管钙化的相对危险因素。

外周血Lp-PLA2和FGF23水平变化与脑梗死后认知功能障碍的相关性

目的分析外周血脂蛋白相关磷脂酶A2(Lp-PLA2)、成纤维细胞生长因子23(FGF23)水平变化与脑梗死后患者认知功能障碍的相关性。方法选取2019-04—2022-12邯郸市中心医院收治的160例脑梗死患者为研究对象,根据患者是否发生认知功能障碍分为认知障碍组和非认知障碍组,对比2组基线资料及外周血Lp-PLA2、FGF23水平,并采用Logistic回归分析患者发生认知功能障碍的影响因素,采用Pearson相关性分析外周血Lp-PLA2、FGF23与简易智力状态评价量表(MMSE)评分的关系,采用ROC曲线评估外周血Lp-PLA2、FGF23对脑梗死后患者认知功能障碍的预测价值。结果160例脑梗死患者中,48例(30.00%)发生认知功能障碍。认知障碍组患者的平均年龄、高血压、糖尿病、吸烟、文化程度、MMSE评分及血清Lp-PLA2、FGF23水平等方面与非认知障碍组相比,差异有统计学意义(P<0.05)。Logistic回归分析显示,年龄、高血压、糖尿病、吸烟、文化程度低及血清Lp-PLA2、FGF23水平升高是影响脑梗死后认知功能障碍发生的独立危险因素(P<0.05)。Pearson相关性分析显示,脑梗死患者血清Lp-PLA2、FGF23水平与MMSE评分呈负相关(P<0.05)。ROC曲线显示,Lp-PLA2的曲线下面积为0.770,FGF23的曲线下面积为0.779,联合检测的曲线下面积为0.873(P<0.05),表示两者联合检测可作为评价脑梗死后认知功能障碍的有效指标。结论Lp-PLA2、FGF23在脑梗死后认知功能障碍患者血清中均呈高表达,二者联合检测有助于提高对脑梗死后认知功能障碍的预测价值。

维持性血液透析患者口服小剂量骨化三醇对FGF-23及血管钙化的影响

目的探讨维持性血液透析(Maintenance hemodialysis,MHD)患者血清FGF-23水平与血管钙化的关系及口服小剂量骨化三醇对成纤维细胞生长因子-23(Fibroblast growth factor-23,FGF-23)及血管钙化的影响。方法选择MHD患者63例,其中已口服小剂量骨化三醇治疗3个月以上的患者有33例(占52.38%)。用ELISA法检测FGF-23,化验肝肾功能、血糖血脂、甲状旁腺素(i PTH)、铁蛋白(FER)和超敏C-反应蛋白(hs CRP),用彩色超声仪检测有无心肌及瓣膜钙化、颈动脉内膜中层厚度(IMT)及有无动脉斑块形成,腰椎侧位X片查腹主动脉钙化。统计学处理采用SPSS17.0统计软件包,以P<0.05为差异有统计学意义。结果 63例MHD患者中有不同部位血管钙化的31例(钙化组)。多因素logistic回归分析血管钙化的危险因素显示:年龄(OR=1.066,P=0.163)、hs CRP(OR=1.195,P=0.065)、钙磷乘积(OR=1.154,P=0.011)、FGF-23(OR=1.048,P=0.012)是发生血管钙化的主要危险因素,高水平的ALB(OR=0.575,P=0.0.016)和口服骨化三醇(OR=0.004,P=0.006)为保护性因素。结论小剂量骨化三醇治疗对FGF-23无明显影响,可能减轻血管钙化。

HFHD对尿毒症患者FGF-23、iPTH水平及心肺功能的影响

目的探讨高通量血液透析(HFHD)对尿毒症患者血清成纤维细胞生长因子-23(FGF-23)、全段甲状旁腺激素(i PTH)水平及心肺功能的影响。方法选取在我院实施血液透析治疗的78例尿毒症患者,采用随机数字表法分为常规组和研究组各39例,收治时间2015年1月-2016年12月,常规组应用常规血液透析治疗,研究组采用HFHD方法治疗,均每周透析3次,2个月后实施效果对比。结果治疗前,常规组和研究组的肺功能指标VC、FVC、TLC及RV差异无统计学意义(P>0.05);治疗后,研究组的VC、FVC、TLC显著高于常规组(P<0.05),研究组的RV显著的低于常规组(P<0.05);治疗前,常规组和研究组的血清FGF-23、iPTH水平差异无统计学意义(P>0.05);治疗后,研究组的血清FGF-23、iPTH水平显著的低于常规组(P<0.05);治疗前,常规组和研究组的BNP、LVEF、LVEDd、LVESD、E/A差异无统计学意义(P>0.05);治疗后,研究组的BNP、LVEDd、LVESD显著的低于常规组(P<0.05),研究组的LVEF值显著的高于常规组(P<0.05)。结论 HFHD有利于改善尿毒症患者肺功能、心功能,同时降低血清FGF-23、i PTH的水平。

心房颤动患者血清FGF-23、miR-208b的表达水平及临床意义

目的探讨血清成纤维细胞生长因子23(FGF23)、miR-208b在心房颤动患者中的表达水平及临床意义。方法选取2018年5月至2019年10月在西安市第三医院治疗的心房颤动患者240例(观察组),其中阵发性房颤患者134例,持续性房颤患者106例;同时选取同期窦性心律健康体检者150例作为对照组。检测并比较两组受检者以及阵发性房颤患者和持续性房颤患者的血清FGF-23、miR-208b水平;采用超声心动图检查观察组患者的心脏参数,分析FGF-23、miR-208b与LAD的相关性。结果观察组患者的血清FGF-23、miR-208b相对表达量分别为(210.20±89.60)ng/mL和5.30±1.22,明显高于对照组的(110.04±32.29)ng/mL和2.90±0.88,差异均有统计学意义(P<0.05);观察组中的持续性房颤患者的血清FGF-23、miR-208b相对表达量分别为(234.22±70.05)ng/mL和5.83±1.00,明显高于阵发性房颤患者的(191.20±65.59)ng/mL和4.88±1.02,差异均有统计学意义(P<0.05);持续性房颤患者的左房直径(LAD)为(38.81±5.11)mm,明显长于阵发性房颤患者的(34.03±4.02)mm,差异有统计学意义(P<0.05);血清FGF-23、miR-208b相对表达量与LAD呈正相关(r=0.411,0.382,P<0.05);观察组患者中主要心血管事件(MACE)患者的血清FGF-23和miR-208b分别为(243.30±72.29)ng/mL和6.12±1.12,明显高于非MACE患者的(199.65±71.43)ng/mL和5.04±1.07,差异均有统计学意义(P<0.05)。结论心房颤动患者血清FGF-23,miR-208b明显升高,且与疾病类型、心脏参数及预后有一定相关性。

血清FGF-23、sKL检测对持续非卧床腹膜透析患者心脏瓣膜钙化的预测价值

目的探讨血清成纤维生长因子23(FGF-23)、可溶性klotho蛋白(sKL)检测对持续非卧床腹膜透析(CAPD)患者心脏瓣膜钙化的预测价值。方法选择CAPD> 3个月的患者109例,根据心脏彩色超声检查的心脏瓣膜钙化情况将其分为瓣膜钙化组51例、瓣膜正常组58例,同期选取30例体检健康者为对照组。采用酶联免疫吸附法检测各组血清FGF-23、sKL水平,采用Logistic回归分析CAPD患者心脏瓣膜钙化的影响因素,用受试者工作特征曲线下面积(AUC)评估血清FGF-23、sKL对心脏瓣膜钙化的预测价值。结果瓣膜钙化组、瓣膜正常组血磷、碱性磷酸酶(ALP)、血钙、血清肌酐(SCr)水平高于对照组(P均<0. 05),总尿素清除指数(Kt/V)低于对照组(P <0. 05);瓣膜钙化组透析龄、血磷、ALP、血钙、SCr、FGF-23水平高于瓣膜正常组(P均<0. 05),Kt/V、血清sKL水平低于瓣膜正常组(P均<0. 05)。血磷、血清FGF-23水平升高是CAPD患者心脏瓣膜钙化的独立危险因素(OR分别为1. 995、2. 328,P均<0. 05),血清sKL水平升高是CAPD患者心脏瓣膜钙化的保护因素(OR=0. 742,P均<0. 05)。血清FGF-23、sKL预测心脏瓣膜钙化的AUC分别为0. 844、0. 814,二者联合检测预测心脏瓣膜钙化的AUC为0. 941。结论血清FGF-23、sKL是CAPD患者发生心脏瓣膜钙化的影响因素,二者联合检测对CAPD患者发生心脏瓣膜钙化的预测价值较高。