Safety profile of 0.0015%tafluprost eye drops in China:a post-marketing observational study

AIM:To investigate the treatment pattern and safety of tafluprost for glaucoma and ocular hypertension(OH)in clinical practice in China.METHODS:This post-marketing observational study included patients who received tafluprost to lower intraocular pressure(IOP)within 30d between September 2017 and March 2020 in 20 hospitals in China.Adverse drug reactions(ADRs)during tafluprost treatment and within 30d after the treatment were collected.RESULTS:A total of 2544 patients were included in this study,of them 58.5%(1488/2544)had primary open angle glaucoma(POAG),21.9%(556/2544)had OH and 19.7%(500/2544)used tafluprost for other reasons.Of 359 ADRs occurred in 10.1%(258/2544)patients,and no serious adverse event occurred.The most common ADR was conjunctival hyperemia(128 ADRs in 124 patients,4.9%).Totally 1670 participants(65.6%)combined tafluprost with carbonic anhydrase inhibitors(CAIs;37.1%,620/1670),sympathomimetics(33.5%,559/1670),β-blockers(33.2%,555/1670),other prostaglandin analogs(PGAs;15.6%,260/1670)and other eye drops(15.1%,253/1670).The highest incidence of conjunctival hyperemia was noted in patients who received tafluprost in combination with other PGAs(23 ADRs in 23 patients,8.8%,23/260)and the lowest was in combination with CAIs(16 ADRs in 16 patients,2.6%,16/620).Tafluprost was applied in primary angle-closure glaucoma(41.6%,208/500),after glaucoma surgery(17.8%,89/500)and after non-glaucoma surgery(15.8%,79/500).CONCLUSION:Tafluprost is safe for POAG and OH,and tolerable when combined with other eye drops and under various clinical circumstances.

Efficacy and safety of 0.0015% tafluprost versus 0.005% latanoprost in primary open angle glaucoma, ocular hypertension: a Meta-analysis

AIM:To evaluate the intraocular pressure(IOP)-lowering efficacy and safety of tafluprost 0.0015%eye drops[benzalkonium chloride(BAK)0.1 mg/mL]compared with that of latanoprost 0.005%eye drops(BAK 0.2 mg/mL)for primary open angle glaucoma(POAG)and ocular hypertension(OHT).METHODS:All the randomized controlled trials(RCTs)about treating POAG and OHT comparing tafluprost and latanoprost were collected by searching PubMed,Embase,Cochrane Library,CNKI and VIP.The outcomes of interest to evaluate the clinical efficacy and adverse effects included IOP and patient-related drop discomfort.RESULTS:Five RCTs involving 888 glaucoma patients were included.The results showed that,1)at the end of the study,no statistically significant differences were observed in IOP reduction[standard mean difference(SMD)=0.48,95%CI 0.07 to 0.88,P=0.085]between tafluprost and latanoprost;2)No statistically significant differences were observed in adverse events of foreign-body sensation[relative risk(RR)=0.62,95%CI 0.26 to 1.46,P=0.269],eye irritation(RR=1.16,95%CI 0.49 to 2.75,P=0.744),eye pain(RR=2.000,95%CI 0.949 to 4.216,P=0.07),iris hyperpigmentation(RR=0.741,95%CI 0.235 to 2.334,P=0.61),dry eye(RR=1.154,95%CI 0.409 to 3.256,P=0.79)and eye pruritus(RR=1.600,95%CI 0.536 to 4.774,P=0.4)between tafluprost and latanoprost.However,tafluprost showed more reported incidence of conjunctival hyperaemia than latanoprost(RR=2.11,95%CI 1.24 to 3.59,P=0.006).CONCLUSION:Tafluprost 0.0015%eye drops(BAK 0.1 mg/mL)and latanoprost 0.005%eye drops(BAK 0.2 mg/mL)are comparable in lowering IOP for open angle glaucoma(OAG)and OHT.It does not differ in the incidence of foreign-body sensation,eye irritation,eye pain,iris hyper-pigmentation,dry eye and eye pruritus,but tafluprost shows less ocular tolerability because of more incidence of conjunctival hyperaemia.

Switching Study of Tafluprost/Timolol Fixed-Combination Ophthalmic Solution, Following Unfixed Combination of Tafluprost Ophthalmic Solution 0.0015% and Timolol Ophthalmic Gel-Forming Solution 0.5%

Purpose: Fixed-combination medication to treat glaucoma can reduce intraocular pressure (IOP) without negative effects of concomitant medication. Tafluprost/timolol fixed-combination ophthalmic solution (TTFC) has been reported to show similar effectiveness in lowering IOP, compared with concomitant use of its component drugs, tafluprost and timolol. However, the difference in IOP-lowering effects between TTFC and concomitant use of tafluprost and gel-forming timolol is unknown. Hence, we conducted this switching study from tafluprost and gel-forming timolol to TTFC in glaucoma patients undergoing multi-drug therapy. Design: Multi-center, open-label, interventional clinical study. Methods: Twenty-eight patients (28 eyes;safety analysis set) with primary open-angle glaucoma and ocular hypertension, who had completed the 4-week-concomitant phase of tafluprost and gel-forming timolol, were treated for 8 weeks with TTFC. IOP, adherence, ocular surface safety, and the usability of ophthalmic solution were compared before and after switching. This study was approved by the ethics committees of Kitasato University Hospital and all other study sites. All patients provided written informed consent to participate. Results: IOP at 8 weeks after switching was significantly lower than before switching (P = 0.0001) in the efficacy analysis set (n = 24). The self-reported adherence rate remained high after switching;moreover, there was no meaningful change in ocular surface safety. Patient questionnaires regarding usability of medication revealed that 85.7% of patients preferred their instillation prescription after switching, including TTFC. Among the safety analysis set (n = 28), no adverse events were reported in relation to the study drug. Conclusion: TTFC showed greater IOP reduction than concomitant therapy. Thus, TTFC may be a better option in glaucoma patients than concomitant therapy.

他氟前列素在青光眼治疗中的神经保护作用及其分子机制

青光眼是一种以视网膜神经节细胞(retinal ganglion cell,RGC)及其轴突的进行性变性和丢失为主要特征的眼病,是导致视力丧失的最常见原因。尽管其具体的发病机制尚未完全明确,但众所周知,眼内压升高是青光眼进展的主要危险因素。目前,通过药物和手术治疗降低眼内压是控制疾病进展的主要手段。他氟前列素因其能有效长期稳定地降低眼内压,且不良反应轻微、患者依从性高、无明显全身不良反应,已成为治疗原发性开角型青光眼及眼高压症的一线治疗药物。近年来的研究表明,他氟前列素除了具有降低眼内压的效果外,还可能具有神经保护作用。文章对他氟前列素的药理作用及其在神经保护方面的潜在效益进行综述,为开发更有效的治疗青光眼药物提供理论依据和科研基础。然而,目前缺乏充分的临床研究证据支持其神经保护效应,未来研究应进一步探索这一领域,以促进针对视神经保护的药物开发和基于视神经再生的视觉功能重建。

抗青光眼药Tafluprost

青光眼是一种常见眼疾，目前尚无法治愈，但可通过早期的诊断和治疗，防止其进一步恶化甚至致盲。高眼压被认为是青光眼发病的主要风险因素之一，也是可经临床干预而缓解的少数症状之一，因此对青光眼的治疗通常都是从降低眼压着手，以防视神经损伤并维持视力。

他氟前列素治疗开角型青光眼的疗效观察

目的探讨他氟前列素滴眼液对初始用药、单药或多种药物降压控制不佳的开角型青光眼患者的降眼压疗效。方法将66例116眼诊断为原发性开角型青光眼患者纳入本研究,分为首选治疗组18例36眼、联合用药组26例38眼和替换治疗组22例42眼。每晚使用他氟前列素滴眼液1次,每次一滴。在治疗前以及治疗后4周和12周进行Goldmann压平眼压计测量眼压,测量时间均为早上8-9点;进行视力、裂隙灯下眼前段检查、角膜荧光素染色及眼底镜检查;在用药前与治疗后12周行Humphery视野检查,记录各组结果并进行相关统计学分析。结果首选治疗组治疗前眼压为(24.6±3.6)mm Hg(1 k Pa=7.5 mm Hg);治疗后4周和12周眼压分别为(18.8±1.5)mm Hg、(18.6±1.7)mm Hg,分别下降(5.7±2.1)mm Hg、(6.1±2.3)mm Hg,与治疗前比较,差异均有统计学意义(t=14.365、17.238;均为P<0.001)。联合用药组治疗前眼压为(25.7±5.7)mm Hg;治疗后4周和12周眼压分别为(18.7±3.4)mm Hg和(17.4±3.2)mm Hg,分别下降(6.6±3.5)mm Hg、(6.8±3.7)mm Hg,与治疗前比较,差异均有统计学意义(t=12.840、13.365;均为P<0.001)。替换治疗组治疗前眼压为(22.8±5.6)mm Hg;治疗后4周和12周眼压分别为(17.1±3.2)mm Hg、(16.2±2.6)mm Hg,分别下降(5.6±3.8)mm Hg、(6.6±4.2)mm Hg;其中替换β受体阻滞剂与前裂腺素类药物降压治疗,治疗后4周与12周眼压下降幅度在替换β阻滞剂组(5.0±4.1)mm Hg、(6.3±4.1)mm Hg,在替换PG类药物组为(5.8±2.5)mm Hg、(6.4±4.7)mm Hg,治疗后12周同治疗前比较,差异均有统计学意义(t=12.095、13.070;均为P<0.001)。共有7眼患者出现不良反应,为轻到中度结膜充血,未见角膜染色。治疗前视野缺损为(5.4±1.8)d B,治疗后12周为(5.6±1.4)d B,治疗前后差异无统计学意义(P>0.05)。结论他氟前列素滴眼液能有效降低原发性开角型青光眼患者的眼压;对首选用药、替代治疗及联合用药,他氟前列素滴眼液均能有效控制眼压。

他氟前列素等前列腺素类药物用于青光眼治疗的药物经济学分析

目的:研究药物经济学评价对降低青光眼治疗成本、促进临床合理用药的重要性。内容与方法:分析比较他氟前列素与其他前列腺素类药物治疗青光眼的有效性和安全性,从药物经济学评价和上市后影响预测两个角度分析应用他氟前列素的经济性。结论 :药物经济学评价对优化青光眼治疗方案、控制药品费用、减轻患者费用负担具有重要意义。

他氟前列素滴眼液联合盐酸卡替洛尔滴眼液治疗开角型青光眼的临床效果

目的探讨他氟前列素滴眼液联合盐酸卡替洛尔滴眼液治疗开角型青光眼的临床效果。方法选取2016年5月至2019年10本院收治的120例开角型青光眼患者作为研究对象,随机将其分为对照组(60例120只患眼,盐酸卡替洛尔滴眼液)和观察组(60例120只患眼,他氟前列素滴眼液联合盐酸卡替洛尔滴眼液)。比较两组的临床疗效、眼压变化情况、眼血流动力学指标及视觉功能评分。结果观察组的治疗总有效率高于对照组(P<0.05)。治疗后1、2、3个月,两组眼压均降低,且观察组低于对照组(P<0.05)。治疗后,两组EDV、PSV及各项NEI-VFQ-25评分均升高,RI均下降,且观察组优于对照组(P<0.05)。结论他氟前列素滴眼液联合盐酸卡替洛尔滴眼液治疗开角型青光眼患者的疗效显著,能够有效改善患者眼压及眼血流动力学指标水平,提高患者视觉功能,值得临床推广应用。

Long-term assessment of prostaglandin analogs and timolol fixed combinations vs prostaglandin analogs monotherapy

AIM： To draw a Meta-analysis over the comparison of the intraocular pressure （lOP）-lowering efficacy and safety between the commonly used fixed-combinations of prostaglandin analogs and 0.5% timolol with prostaglandin analogs （PGAs） monotherapy. METHODS： After searching the published reports from MEDLINE, EMBASE, the Cochrane Library, all randomized controlled clinical trials （RCTs） comparing the fixed combination of PGAs/timolol therapy （FCs） and PGAs monotherapy with treatment duration at least 6mo were included. The efficacy outcomes were mean diurnal lOP, percentage of participants whose lOP were lower than 18 mm Hg, incidence of visual field change, while the safety outcomes included corneal side effects, hyperemia and eye irritation. The analysis was carried out in RevMan version 5.3 software. RESULTS： After six-month medical intervention, the mean diurnal lOP of FCs was lower than PGAs （MD -1.14, 95% CI -1.82 to -0.46, P=0.001）; the percentage of target lOP achieving between FCs and PGAs showed no significant difference （RR 1.18, 95% Cl 0.97 to 1.43, P=0.10）. No statistically significant differences of the incidence of hyperemia （RR 0.67, 95% CI 0.45 to 1.01, p=0.06） and eye irritation （RR 1.20, 95% CI 0.95 to 1.51, P=0.12） between the FCs and PGAs monotherapy were detected. Only one research involved in corneal events, result of this trial revealed no difference between two intervention groups regarding corneal effects （central endothelial cell density, MD -0.20, 95% CI -0.72 to 0.32, P=0.45; central corneal thickness, MD -0.01, 95% Cl -0.02 to 0.00, P=0.23）. The evaluation of visual field change was not performed due to the limited duration of the trials included in this Meta-analysis. CONCLUSION： The long-term efficacy of the FCs overweighed the PGAs monotherapy in lowering lOP, but in the incidence of hyperemia and eye irritation syndromes, the differences are not statically significant. More RCTs with detailed and authentic data over the assessments of visual functions and morphology of optic nerve heads are hoped to be conducted.

他氟前列素的合成工艺改进

以科立内酯为起始原料,经过Swern氧化反应、Hormer-Wadsworth-Emmons反应、氟代、水解、还原、Wittig反应、酯化等反应合成目标化合物,总收率为47.2%,目标化合物和关键中间体结构经MS和1H NMR确证。本工艺改进提高了反应收率,减少了过柱提纯的步骤,降低了生产成本,有利于工业化生产。

他氟前列素合成纵览

目的通过对已有的他氟前列素的合成方法进行分析总结,找到价格低廉,减少污染,更适合工业化生产的合成路线。方法对他氟前列素合成方法的总结,整理,归纳。结果与结论以23为反应原料,反应成本低,绿色环保,适合工业化生产。

他氟前列素的结构确证

目的建立确立他氟前列素化学结构的方法。方法通过红外光谱、质谱和核磁共振波谱对他氟前列素进行结构分析。结果通过高分辨质谱确定了他氟前列素的分子式,红外光谱显示出各基团的特征吸收,通过1H-NMR、1H-1H COSY、13C-NMR、DEPT、HSQC和HMBC等手段,明确归属了其所有的碳氢信号峰。结论根据谱学特征确证了他氟前列素的化学结构,该方法准确可行,可为他氟前列素的化学结构鉴定提供依据。

他氟前列素治疗青光眼和高眼压症的真实世界研究

药物治疗是青光眼常见的降眼压措施,多个指南或共识一致推荐前列腺素衍生物为治疗青光眼的首选药物。真实世界研究(RWS)是指在真实临床、社区或家庭环境下获取多种数据,从而评价某种治疗措施对患者健康真实影响的观察性研究,RWS显示他氟前列素对原发性开角型青光眼、高眼压症、正常眼压性青光眼和其他各种类型青光眼均有良好的降眼压效果,在单药初治、换药治疗及联合治疗的治疗模式下均可降低各类型青光眼或高眼压症患者的眼压,且眼部不良反应较轻。然而目前相关的RWS还存在无对照组等局限性,未来还需要进一步研究,评估其药物应用效果。本文就他氟前列素治疗不同类型青光眼及高眼压症患者的RWS概览及在不同治疗模式下的疗效和他氟前列素在RWS中的安全性、依从性进行综述,以期为他氟前列素实际的临床应用提供一定的指导。

他氟前列素滴眼液治疗正常眼压性青光眼的临床效果观察

目的评价他氟前列素滴眼液对正常眼压性青光眼(normal tension glaucoma,NTG)的临床治疗效果及安全性。方法采用前瞻性队列研究方法,选择2019年1月1日至2020年8月31日在首都医科大学附属北京同仁医院眼科首诊的NTG患者56例,随机选取1只眼作为研究眼,入选后给予他氟前列素滴眼液治疗,连续3个月。比较用药前后的眼压、最佳矫正视力、视野平均缺损、视野指数、视盘周围毛细血管密度及视盘周围视网膜神经纤维层平均厚度,并观察药物不良反应的发生情况。结果56例患者中男18例,女38例,平均年龄(45.9±10.7)岁,均为双眼发病。入选的56只眼治疗前平均眼压为(16.67±2.67)mmHg,治疗3个月后平均眼压为(13.52±2.08)mmHg,平均降低幅度为18.9%,治疗前后比较差异有显著性(P=0.007)。与未接受治疗时的基线眼压相比,有8.93%(5/56)眼的眼压降低幅度≥30%,66.07%(37/56)眼的眼压降低幅度≥15%,其他眼的眼压降低幅度<15%。治疗前后的最佳矫正视力、视野平均缺损、视野指数、视盘周围毛细血管密度、视盘周围视网膜神经纤维层平均厚度比较差异均无显著性(P>0.05)。4例患者出现中度结膜充血或异物感,无其他明显不良反应发生。结论他氟前列素滴眼液可有效降低NTG患者的眼压,结膜充血是其常见并发症。

他氟前列素滴眼液联合明目汤对原发性开角型青光眼眼压及视力的影响

目的探讨他氟前列素滴眼液联合明目汤对原发性开角型青光眼眼压及视力的影响。方法选取2017年6月至2020年6月河南省省立医院收治的82例原发型开角型青光眼患者,采用随机数字表法分为对照组和观察组,每组41例。对照组采用0.015%他氟前列素滴眼液治疗,观察组在对照组基础上口服明目汤治疗,两组均治疗1个月。比较两组治疗前后眼压、视力及视网膜中央动脉(CRA)血流参数变化,并评价其临床疗效。结果观察组治疗后眼压低于对照组,而视力好于对照组,差异有统计学意义(P<0.05)。观察组治疗后CRA中的收缩期血流峰值速度、舒张末期血流速度大于对照组,而阻力指数低于对照组,差异有统计学意义(P<0.05)。观察组治疗后治愈率、总有效率均高于对照组,差异有统计学意义(P<0.05)。结论他氟前列素滴眼液联合明目汤能够进一步提高原发性开角型青光眼的临床疗效,改善患者的眼压及视力。

0.0015%他氟前列素滴眼液对原发性开角型青光眼患者眼压、眼血流动力学及血清细胞因子的影响

目的探讨0.0015%他氟前列素滴眼液对原发性开角型青光眼患者眼压、眼血流动力学及血清细胞因子的影响。方法选取2015年5月~2017年4月于我院眼科就诊的86例原发性开角型青光眼患者为研究对象。按照随机数表法将所选患者分为对照组,观察组,各43例;对照组患者运用马来酸噻吗洛尔滴眼液进行滴眼治疗,观察组患者采用0.0015%他氟前列素进行滴眼治疗,对比两组治疗前后眼压(IOP)、视网膜中动脉(CRA)、睫状体后动脉(PCA)眼血流动力学指标变化;以及IL-4、IL-6、IL-12等细胞因子水平变化。结果 (1)治疗前两组患者IOP无明显差异(P>0.05),随着治疗时间的延长,两组患者的IOP均明显下降,且观察组患者明显低于对照组(P<0.05);(2)治疗后两组CRA、PCA血流动力学指标较治疗前均有差异(P<0.05),治疗后PSV、EDV上升,RI下降,但对照组PSV、EDV上升程度以及RI下降程度均低于观察组(P<0.05);(3)治疗前两组IL-4、IL-6、IL-12水平比较无明显差异(P>0.05),治疗后两组IL-4水平明显下降,且观察组明显对于对照组(P<0.05),治疗后IL-6、IL-12水平明显上升,观察组明显高于对照组(P<0.05)。结论 0.0015%的他氟前列素治疗原发性开角型青光眼患者,其降眼压效果良好,安全性高,同时还可以改善患者的局部免疫水平。

他氟前列素联合派立噻治疗开角型青光眼的临床疗效

目的探讨应用他氟前列素联合派立噻治疗开角型青光眼的临床疗效。方法便利选取该院于2017年1月-2021年8月门诊诊疗的56例(56眼)开角型青光眼患者,随机分为对照组与观察组,各28例(28眼)。对照组应用派立噻滴眼液进行治疗,观察组在此基础上加用他氟前列素滴眼液,应用1个月后,对比观察两组患者眼压的变化情况、治疗有效率、各象限(上方、下方、鼻侧、颞侧)及平均RNFL厚度。结果观察组的治疗有效率为100.00%,对照组为78.57%,数据对比差异有统计学意义(χ^(2)=4.667,P<0.05);治疗前,两组患者眼压分别为(33.15±4.35)、(32.18±4.26)mmHg,差异无统计学意义(t=0.843,P>0.05),治疗后,观察组患者眼压为(14.64±2.36)mmHg,对照组患者眼压为(20.15±2.16)mmHg,观察组的眼压值明显小于对照组,差异有统计学意义(t=9.113,P<0.05);治疗后,观察组各象限(上方、下方、鼻侧、颞侧、平均值)RNFL厚度分别为(96.37±14.25)、(97.71±15.08)、(101.37±14.25)、(102.25±15.34)、(100.83±16.58)μm,均大于对照组的(87.12±13.25)、(89.13±12.91)、(90.05±13.80)、(91.14±14.42)、(89.24±14.33)μm,差异有统计学意义(t=2.515、2.287、3.020、2.792、2.799,P<0.05)。结论采用他氟前列素联合派立噻滴眼液治疗开角型青光眼比单纯应用派立噻更能有效的提高治疗效果,更显著的降低眼压,保护视神经纤维层,使其厚度减少缓慢,具有较高的临床应用价值,值得推广。

前列腺素类药物治疗眼压升高患者的贝叶斯网状Meta分析

目的:系统评价前列腺素类药物在降低眼压方面的疗效及安全性。方法:计算机检索中国知网、CBM、万方、维普、PubMed、Cochrane Library等数据库,检索关于前列腺类药物治疗眼压升高患者的随机对照试验(randomized controlled trial, RCT),检索时限为建库至2022年4月。采用Cochrane推荐的偏倚风险评估工具对纳入RCT进行质量评价。应用RevMan 5.4、Stata 14、ADDIS软件进行贝叶斯网状Meta分析。结果:纳入25篇RCT,总样本量3 688例,研究时限为3个月,纳入4种前列腺类药物,拉坦前列素(latanoprost, LAT)、贝美前列素(bimatoprost, BIM)、曲伏前列素(travoprost, TRA)、他氟前列素(tafluprost, TAF)。有效性方面,降低眼压效果排序为BIM>TAF>LAT>TRA。结膜充血发生率排序为BIM>TRA>TAF>LAT。结论:根据本研究结果,对于病情严重患者,如能耐受结膜充血等局部副作用应用贝美前列素是最优选择,对于单纯高眼压症及轻度青光眼患者,应用他氟前列素和拉坦前列素即可获得稳定降眼压效果,且助于提高用药依从性。

天津市眼科医院眼科药物评价标准的建立与应用

目的建立眼科药物评价标准并将其应用于天津市眼科医院眼科临时采购药品评价。方法围绕药品的安全性、有效性、经济性、创新性、适宜性和可及性6个维度,制定眼科药物评价标准,并对天津市眼科医院2021—2022年临时采购的眼用药品进行回顾性评价。结果制定了百分制“眼科药品临床综合评价表”,临时采购的9种眼用药品评分均高于60分。结论“眼科药品临床综合评价表”可作为天津市眼科医院药品临床评价的参考依据,有助于提高医院药事管理能力及合理用药水平。

他氟前列素滴眼液治疗青光眼的应用研究进展

他氟前列素是一种具有强前列腺素F受体亲和力的前列腺素类似物(prosaglandin analogues,PGA),2003年首次报告,2008年作为首个原研无防腐剂的PGA药剂上市,以显著的降眼压能力被用于治疗开角型青光眼和高眼压症的一线药物。其独特的双氟原子结构赋予其强代谢稳定性,使其以低于其他PGA滴眼液的药物浓度发挥同等的疗效。大量临床研究证实了其降眼压疗效,不良反应发生较少且程度较轻。除降眼压外,还具有一定的改善眼血流量、视神经保护以及对其他眼组织的保护作用。近年来许多临床试验聚焦于无防腐剂他氟前列素滴眼液关于眼表安全性的评估。2022年无防腐剂他氟前列素滴眼液进入我国临床。本文对他氟前列素的发现、药理学机制和药代动力学进行介绍,并总结无防腐剂他氟前列素滴眼液的临床疗效、安全性和耐受性,以期为其临床使用提供指导。