Outcomes of long-acting injectable antipsychotics use in pregnancy:A literature review

BACKGROUND Women with a history of serious psychotic disorders are at increased risk of disease relapse during pregnancy.Long-acting injectable(LAI)antipsychotics have been widely used to improve adherence and prevent relapse in patients with various severe psychotic disorders,but there is a lack of high-quality data from previous research on the safety of LAI antipsychotics during pregnancy.AIM To summarize relevant data on maternal,pregnancy,neonatal,and developmental outcomes from published cases of LAI antipsychotic use in pregnancy.METHODS A literature search was performed through November 11,2023,using three online databases:PubMed/MEDLINE,Scopus,and Web of Science.Case reports or case series that reported information about the outcomes of pregnancy in women who used LAI antipsychotics at any point in pregnancy,with available full texts,were included.Descriptive statistics,narrative summation,and tabulation of the extracted data were performed.RESULTS A total of 19 publications satisfied the inclusion criteria:3 case series,15 case reports,and 1 conference abstract.They reported the outcomes of LAI antipsychotic use in 74 women and 77 pregnancies.The use of secondgeneration LAI antipsychotics was reported in the majority(n=47;61.0%)of pregnancies.First-generation LAI antipsychotics were administered during 30 pregnancies(39.0%).Most of the women(approximately 64%)had either satisfactory control of symptoms or no information about relapse,while approximately 12%of them had developed gestational diabetes mellitus.A minority of cases reported adverse outcomes such as stillbirth,spontaneous abortion,preterm birth,low birth weight,congenital anomalies,and neurological manifestations in newborns.However,there were no reports of negative long-term developmental outcomes.CONCLUSION Currently available data seem reassuring,but further well-designed studies are required to properly evaluate the risks and benefits of LAI antipsychotic use during pregnancy.

Optimal needle insertion length for intramuscular injection of risperidone long-acting injectable (RLAI)

Risperidone long-acting injectable (RLAI) is approved for the treatment of schizophrenia in many countries. The suggested site is the gluteal muscle with a needle length of two inches (50 mm) in Japan, which is longer than the ordinarily used needle for intramuscular injections. The aim of this study was to determine the optimal needle insertion length for accurate delivery of RLAI procedure among subjects who have normal body mass index (BMI: 18 to 25) and high BMI (>25). Thirty-seven patients with schizophrenia were administered RLAI intramuscularly into the dorsogluteal muscle. The standard procedure required inserting 80% of the two inch needle. By using data collected by ultrasonography, the findings confirmed that the median needle insertion lengths for subjects with normal and high BMI were 39.0 and 45.5 mm, respectively. To deliver RLAI effectively and safely, the authors strongly recommend that a specialized needle be used that is “marked” at the 40 mm point from the tip of the needle to the base. In this way regardless of subcutaneous fat content, the RLAI can be safely delivered into the muscle without causing untoward or side effects.

Effects of Depth of Needle Insertion with Risperidone Long-Acting Injectable in Persons with Schizophrenia: A Randomized Double-Blind Study

In some cases, if the insertion depth is shallower than expected, intramuscular (IM) injection of risperidone long-acting injectable (RLAI) may not penetrate the muscle fascia. However, if needle insertion depth is deeper than anticipated, needle penetration may cause damage to nerves, arteries and veins. Few clinical studies were done to evaluate the depth of needle length insertion reaching the intended gluteal muscle. The aim of this study was to evaluate the suitable depth of injecting RLAI. Twenty-six patients with schizophrenia were treated with RLAI, and randomly divided into two groups: 50 mm needle inserted group (Group-D, deep insertion, n = 13) and 20 mm needle insertion group (Group-S, shallow insertion, n = 13). For Group-S, the needle length was marked with a spacer at exactly 20 mm. Injections were performed by the psychiatrist or nurse, alternating between the two gluteal sites by double-cross method every two weeks. Clinical psychotic symptoms and injection site reactions were recorded throughout the study period. Experienced psychologists who were blinded from the needle-length experimental variable evaluated patients’ psychotic symptoms using the Positive and Negative Syndrome Scale (PANSS) every two weeks. The plasma 9-hydroxyrisperidone (9-OH-RIS) concentrations were measured every two weeks;comparison data were determined on the 8th week and the 14th week. No significant difference was observed in 9-OH-RIS concentrations, psychotic symptoms, injection site skin reactions of subjects in both groups. However, in Group-D, injection site adverse reactions were confirmed in two subjects (15%). In Group-S, injection site reactions were confirmed in six subjects (46%). Although effective 9-OH-RIS concentrations were obtained with the insertion using both depth, it was concluded that the 50 mm insertion length was more suitable for dorsogluteal IM injections in adult patients with schizophrenia as demonstrated by the incidence of local adverse skin reactions.

Long-Term Clinical Outcome of Patients Using Risperidone Long-Acting Injectable: The Romanian e-STAR Database

The objectives of e-STAR Romania (NCT00283517) were to collect clinical outcome data of Romania schizophrenia or schizo-affective disorder patients;prospectively to assess the reasons of treatment initiation, medication usage patterns;to document (long-term) clinical efficacy;and to collect safety data, as well as recording 2-year corresponding retrospective data. In total, 378 eligible subjects were enrolled who were initiated either on risperidone long-acting injectable (RLAI) (290) or on an oral antipsychotic (OA) (88) at baseline as required by the local Summary of the Product Characteristics. Data were collected from per patient both retrospectively and prospectively over a 24-month period at 3-month intervals after starting treatment. The results indicated that subjects suffering from schizophrenia or schizo-affective disorder initiated on RLAI were less likely to be hospitalized within the first 24 months after the initiation of treatment. Moreover, subjects treated with RLAI experienced significant improvements in their illness severity and functioning. Discontinuation rates for RLAI were low and doses were stable throughout the 24 months following the initiation of treatment. In addition, the necessity for supplementary concomitant medication was reduced. Adverse events were reported in 20.3% (RLAI) and 11.4% (OA) of the subjects. In general, patients initiated on RLAI and OA at baseline both clinically improved on all assessed parameters but a larger improvement was observed for patients on RLAI. Incidences of reported AEs during the use of RLAI in a naturalistic setting are comparable with those described in clinical studies;however, the incidence of extrapyramidal signs and weight gain was lower than expected.

Intramuscular Diffusion Status of Risperidone and Aripiprazole Long Acting Injectable (LAI) by Ultrasonography

The aim of this study was to consider the characteristics of intramuscular diffusion status of risperidone and aripiprazole long acting injectable (LAI) by ultrasonography. Subjects were 40 adult subjects diagnosed with schizophrenia and treated with LAI [32 patients were risperidone LAI (RLAI) and 8 patients were aripiprazole LAI (ALAI)]. However, in this paper, only three cases (one RLAI case and 2 ALAI cases) were selected to illustrate the diffusion effects of both LAI. Dorsogluteal intramuscular (IM) injection sites were measured at prone position using the “double cross” method. Before LAI injection, the distance from the epidermis to the under-fascia (DEUF), and distance from the epidermis to the iliac bone (DEI) at the IM injection site were assessed by using ultrasonography: 1) the injection needle was inserted to the gluteus medius, and 2) observed the diffusion status within the muscle injected RLAI and ALAI were confirmed using the B-mode ultrasonography. Both RLAI and ALAI were depicted as high echogenicity with acoustic shadowing. It was considered that the diffusion states of LAIs by ultrasonography were important time course evaluations providing objective evidence.

Pharmacokinetics,pharmacodynamics and safety of a single-dose long-acting Risperidone injection in Chinese patients with schizophrenia

In the present study,we aimed to determine the pharmacokinetics(PK),pharmacodynamics(PD),adverse events(AEs),and their relationships in Chinese patients with schizophrenia after a single dose of long-acting risperidone.Schizophrenic patients(six females and seven males)were enrolled in this study.Serial blood samples were collected after drug administration during 63 d,and the drug concentrations were analyzed by LC-MS/MS.Safety and tolerance were evaluated by monitoring the AEs,changes in clinical laboratory results,12-lead ECG,vital signs,physical examination,and injection-site reactions.The extrapyramidal symptoms were evaluated using the ESRS.Efficacy was evaluated by the PANSS and BPRS.Twelve out of the 13 participants completed the trial.There were few clinically meaningful changes in mean clinical laboratory values,vital signs,or ECG parameters,except for the prolactin level and body weight.There were no serious AEs,and those observed were reversible.Significant clinical improvements in PANSS and PANSS-derived BPRS total scores were observed.The mean(standard deviation,coefficient of variation)values for these PK parameters were as follows:C_(max),8.954(8.059,90.0%)ng/mL;area under the curve AUC_(0-t),2453(1156,47.1%)ng·h/mL;AUC_(0-∞),2472(1160,46.9%)ng·h/mL;t_(max),830.0(min:744.0,max:984.0,11.8%)h;and t_(1/2),68.56(10.77,15.7%)h.The PK characteristics of long-acting risperidone showed a high level of inter-individual variation,while there were no clear correlations between PK,efficacy and AEs among the patients in the present study.

注射用利培酮微球(Ⅱ)治疗急性期精神分裂症患者的疗效及安全性研究

背景长效抗精神病药是目前精神分裂症全病程治疗中的重要选择之一。注射用利培酮微球(Ⅱ)在剂型上进行了改良,治疗期间无需补充口服药物,能够快速起效,但目前尚缺少其临床疗效的相关研究。目的评估注射用利培酮微球(Ⅱ)治疗急性期精神分裂症患者的疗效及安全性。方法本研究为单臂多中心前瞻性研究,纳入2021年8月—2022年4月北京大学第六医院、河北省精神卫生中心、乌鲁木齐市第四人民医院、太原市精神病医院、天津市安定医院5个研究中心,18~55岁急性期精神分裂症患者为研究对象,给予25.0 mg/2周、37.5 mg/2周或50.0mg/2周可变剂量注射用利培酮微球(Ⅱ)治疗,随访8周。分别在基线和2、4、6、8周末进行阳性与阴性症状量表(PANSS)、临床总体印象量表(CGI)及精神科药物不良反应量表(UKU)评定。于基线及8周末进行个人和社会功能量表(PSP)评定,并采集患者实验室检查指标。结果研究共纳入58例患者。治疗2、4、6、8周末患者PANSS总分、阳性症状量表分、阴性症状量表分、一般精神病理量表分、CGI-疾病严重程度(CGI-S)评分均较基线降低(P<0.001);2、4、6周及8周末患者PANSS总分减分有效率分别为37.9%(22/58)、70.7%(41/58)、89.7%(52/58)和89.7%(52/58)。治疗8周末PSP评分[(71.00±14.99)分]高于基线[(46.28±15.43)分](P<0.001)。患者的平均血药浓度在1、2、4、6、8周末分别达到(12.94±8.47)、(13.23±10.86)、(21.09±13.04)、(23.64±14.23)、(29.08±19.51)μg/L。常见不良反应包括震颤、肌张力障碍、便秘等,均为轻度到中度,无严重不良反应及因无不良反应脱落者。治疗8周末泌乳素水平较基线升高(P<0.05)。结论注射用利培酮微球(Ⅱ)可在不补充口服抗精神病药的情况下快速起效,可有效改善精神分裂症急性期的多维度症状,且耐受性良好。

注射用利培酮微球临床应用专家共识

注射用利培酮微球是我国首个上市临床使用的第二代抗精神病药长效针剂,结合了长效剂型和非典型抗精神病药的优势,临床应用十余年,积累了丰富的临床应用经验,为精神分裂症患者带来更多临床获益。中华医学会精神医学分会精神分裂症协作组组织专家,在2012年《非典型长效针剂(注射用利培酮微球)临床应用专家意见》的基础上,系统汇总国内外最新指南和循证证据,并结合我国临床实践,制定《注射用利培酮微球临床应用专家共识》,旨在提高注射用利培酮微球临床使用的科学性和规范性,为临床医生提供更好的临床用药指导。

注射用长效利培酮微球治疗40例精神分裂症疗效与安全性研究

目的：探讨长效利培酮微球治疗40例精神分裂症8～20周临床疗效与安全性。方法：40例精神分裂症患者随机入组。40例患者使用长效利培酮微球首次剂量均为每2周25mg，随后根据病情变化增加，最大剂量每2周50mg。采用阳性和阴性精神症状评定量表（PANSS）、临床总体印象量表（CGI）评定患者精神症状与疗效变化；副反应量表（TESS）评定不良反应。采用自身对照法，在治疗前与治疗后的4，8，12，16，20周分别评定疗效与不良反应。结果：治疗后第4周PANSS减分率为39．5％；第8周为58％；第12～16周为75．5％；第20周为86．1％。PANSS总分在治疗后4，8，12，16，20周的降低与基线比较其差异均有非常显著性（P〈0．01）。CGI-S评分在治疗后4，8，12，16，20周各个阶段的降低与基线比较其差异均有非常显著性（P〈0．01）。30例患者在治疗前后检测血常规、血生化无异常变化，在单用长效利培酮微球的患者中未见显著的EPS与胆碱能样反应。结论：长效利培酮微球治疗4周末（即第3针）即可起效，3～4周可渐减口服药物剂量。长效利培酮微球具有疗效确切、安全性高的特点。

利培酮微球和利培酮治疗精神分裂症对照研究

目的探寻利培酮微球和利培酮治疗精神分裂症患者的疗效和安全性。方法将160例精神分裂症患者随机分为研究组和对照组各80例,研究组用利培酮微球系统治疗,对照组用利培酮系统治疗,共3个月,在基线和治疗后1、2、3个月末应用阳性和阴性综合征量表(PANSS)、临床疗效总评量表-病情严重程度(CGI-S)、临床疗效总评量表-疗效总评(CGI-I)、锥体外系症状评定量表(ESRS)评价。结果两组在治疗后第1、2、3个月末的PANSS评分均低于基线时相应评分(P<0.05)。在治疗后第2、3个月末,研究组PANSS评分以及CGI评分均低于对照组(P<0.05)。研究组治疗后第1、2、3个月末ESRS评分均低于对照组(P<0.05)。结论利培酮微球可有效、安全地治疗精神分裂症患者。

利培酮长效注射剂的药动学特征和临床应用

微球注射剂系采用生物降解聚合物为骨架将药物包裹于微球内的一种可供注射的剂型,它具有长效、安全和用药方便等优点。现综述国内外刚上市的可缓释2周的利培酮微球注射剂(Risperidal ConstaTM,恒德)的药动学特点和临床应用概况。该制剂用药后可以预测的缓释速率释药和较低血药蜂谷浓度波动,体现了制剂药动学的优点。用阳性和阴性症状量表(PANSS)平均分值评价结果表明,精神分裂症患者采用本制剂进行短期(12周)和长期(12个月)试验治疗,除具有肯定的疗效外,在耐受性和锥体外系不良反应方面也优于利培酮片剂和目前临床其他常规制剂。由于可减少住院次数和发作所需专业机构护理次数以及缩短了累积住院期间,从药物经济学角度考虑也具有较好的优势。

长效利培酮微球治疗精神分裂症的远期疗效研究

目的探讨长效利培酮微球对精神分裂症的远期临床疗效和安全性,以及对血清催乳素的影响。方法于2007年至2009年间入选56例精神分裂症患者,随机分入长效利培酮微球(RLAI)研究组和利培酮口服液(ROS)对照组进行为期1年的治疗,分别以痊愈率、缓解率、停药率、复发率和再住院率进行评价,评定两组的临床总体印象-严重度(CGI-S)与个人和社会功能评分(PSP)量表,并测定血清催乳素水平,以χ2检验和t检验进行统计分析。结果至研究终点时,RLAI组的临床治愈率和缓解率均高于ROS组,无停药、复发或再次住院发生,临床总体印象与个人和社会功能评分改善均优于ROS组。RLAI组血清催乳素水平及总体不良反应发生率均明显低于ROS组(P<0.05)。与ROS组相比,RLAI组无1例发生不依从(P<0.05)。结论长效利培酮微球的远期疗效、安全性及治疗依从性均优于利培酮口服液,适用于维持治疗。

帕利哌酮注射液与利培酮治疗精神分裂症的对照研究

目的：探讨帕利哌酮注射液对精神分裂症患者治疗的疗效及社会功能恢复。方法：对72例精神分裂症患者随机分为两组,每组36人,分别予帕利哌酮注射液（实验组）及利培酮（对照组）治疗,帕立哌酮注射液肌肉注射,首次150mg,1周后予100 mg,此后每4周注射1次,第3次根据情况在75~150 mg之间调整剂量。利培酮采用口服连续给药,每日在4~8 mg之间调整剂量。观察8周,采用BPRS量表评估疗效,采用TESS评估副反应,采用PSP评估社会功能恢复。对于疗效不佳或不能耐受者在8周后换用其他抗精神病药物。结果：两组BPRS量表得分,治疗1周末、2周末、4周末和8周末均与治疗前有显著性差异。治疗组体重平均增加（1.21±1.31）kg,对照组平均增加（3.52±3.21）kg,两组差异有显著统计学意义（P〈0.01）。两组均未见严重不良反应。8周末PSP量表评分治疗组和对照组分别为（69.5±16.31）和（60.5±15.24）分。两组差异有显著统计学意义（P〈0.05）。结论：帕利哌酮注射液对精神分裂症患者治疗效果和不良反应与利培酮相当,但体重增加较少。其独特的给药方式,是减少患者病耻感的有效方式,有利于提高患者治疗依从性,减少中断药物治疗发生的几率。

齐拉西酮注射液治疗精神分裂症急性期症状后续药物的研究

目的:评价精神分裂症急性期激越患者在齐拉西酮注射液治疗3d延用不同口服药物的疗效及安全性。方法:符合ICD-10精神分裂症诊断标准,且急性期注射3d齐拉西酮注射液治疗的患者,随机分配到齐拉西酮试验组(试验组)和利培酮试验组(对照组)各30例,对患者进行基线(最后一针齐拉西酮注射后2 h)评价,以及肌注治疗后的72 h、2周、4周和8周的评价。采用BPRS量表评价主要疗效,采用副反应症状量表(TESS量表)评定药物的不良反应。结果:两组均口服药物治疗2周时,两组BPRS评分有显著性差异(P<0.05),其余时间点两组主要疗效指标差异无统计学意义(P>0.05)。8周时试验组治疗总有效率为80.0%,对照组治疗总有效率为76.7%。试验组药物不良反应较对照组明显减少,TESS量表评分在治疗前后差异无统计学意义(P>0.05);对照组出现锥体外系不良反应、体重增加、月经紊乱较多,治疗前后差异有统计学意义(P<0.05)。结论:甲磺酸齐拉西酮注射液快速有效控制精神分裂症激越症状后,换用齐拉西酮口服疗效与换用利培酮疗效相当,但齐拉西酮安全性更高,不良反应更少。

氯硝西泮对偏执型精神分裂症的辅助治疗作用

目的 :评价利培酮配合氯硝西泮注射液治疗偏执型精神分裂症的疗效。 方法 :对病程 <3年的 80例首次住院 ,选用利培酮治疗的偏执型精神分裂症患者 ,随机分为合用氯硝西泮 (合用组 )和未合用氯硝西泮 (对照组 )各 4 0例 ,进行 8周治疗。采用阳性症状与阴性症状量表 (PANSS)评定疗效 ,副反应量表 (TESS)评定不良反应。 结果 :合用组治疗 2周后PANSS量表总分、阳性症状分、精神病理因子分及症状群中激活性、偏执、攻击性分值均显著下降 ;治疗 4周末时利培酮剂量合用组显著低于对照组。 结论 :利培酮配合氯硝西泮注射液治疗偏执型精神分裂症可缩短疗程 。

长效利培酮微球治疗精神分裂症30例疗效观察

目的:探讨注射用长效利培酮微球治疗精神分裂症的临床疗效和安全性。方法:对30例符合CCMD-3精神分裂症诊断标准的精神分裂症患者随机入组,给予长效利培酮微球(25～50mg/2周)治疗,疗程16周。在治疗前与治疗后的4、8、12、16周末分别用阳性和阴性症状量表(PANSS)、副反应量表(TESS)评定疗效与不良反应,并检测血常规、尿常规、血生化、心电图。对数据进行统计分析。结果:长效利培酮微球治疗后第4周PANSS总分,阳性因子分、阴性阴子分、一般病理分均显著下降,与治疗前比较有显著性差异(P<0.01)。不良反应主要有失眠,轻度体重增加,其它不良反应少见。结论:注射用长效利培酮微球对精神分裂症疗效好,安全性高,依从性好,值得推广。

利培酮口服液合并氯硝西泮治疗精神分裂症急性兴奋的临床研究

目的研究利培酮口服液合并氯硝西泮治疗精神分裂症患者急性兴奋的疗效和安全性。方法将精神分裂症急性兴奋患者87例随机分为两组,治疗组44例予利培酮口服液合并氯硝西泮肌内注射;对照组43例予氟哌啶醇肌内注射,疗程均为7天。采用阳性症状和阴性症状量表(PANSS)评定临床疗效,副作用量表(TESS)评定不良反应。结果治疗7天的疗效相当(P>0.05),治疗组不良反应的发生率明显低于对照组(P<0.05)。结论利培酮口服液合并氯硝西泮治疗精神分裂症急性兴奋疗效肯定,安全性优于氟哌啶醇。

棕榈酸帕利哌酮注射液治疗精神分裂症的临床效果

目的研究棕榈酸帕利哌酮注射液治疗精神分裂症的临床效果。方法72例精神分裂症患者,随机分为观察组与对照组,各36例。观察组患者采用棕榈酸帕利哌酮注射液进行治疗,对照组采用注射用利培酮微球进行治疗。比较两组患者的临床疗效。结果观察组总有效率94.44%明显高于对照组的69.44%,差异有统计学意义(P<0.05)。结论精神分裂症患者通过棕榈酸帕利哌酮注射液治疗,可有效提升整体疗效,改善患者的相关症状,值得推广。

利培酮长效针剂对肇事肇祸精神分裂症患者疗效的研究

目的探讨利培酮长效针剂对肇事肇祸精神分裂症患者的有效性及不良反应。方法对符合ICD-10诊断的43例肇事肇祸精神分裂症患者及43例普通精神分裂症患者进行病例对照研究。在采用利培酮治疗3个月末采用精神病量表(BPRS)和不良反应症状量表(TESS)进行疗效和不良反应评估。结果两组除敌对猜疑因子治疗前得分有明显差异外(P<0.05),两组治疗前或治疗3个月后组间总分及其它各因子评分比较差异均无统计学意义(P>0.05)。组内治疗前后相比,两组各自的总分及各因子得分差异均具统计学意义(P<0.05)。两组组间的不良反应得分及分布差异均无统计学意义(P>0.05)。结论利培酮长效针剂对肇事肇祸精神分裂症患者疗效显著,不良反应较少。

注射用利培酮微球治疗精神分裂症的疗效和安全性分析

目的:探讨注射用利培酮微球治疗精神分裂症的疗效和安全性。方法:收治精神分裂症患者90例,将其平均分为试验组和对照组,对照组采用利培酮片治疗,试验组采用注射利培酮微球治疗。结果:试验组治疗总有效率、生活质量评分明显高于对照组(P<0.05);试验组不良反应发生率明显低于对照组(P<0.05)。结论:注射用利培酮微球治疗精神分裂症的疗效显著且安全性高,有效改善了患者的生活质量。