Toxicity and Viral Load in Urine during Valganciclovir Therapy in Premature Infants

Cytomegalovirus (CMV) infection is the most important cause of mental retardation and sensorineural hearing loss. Antiviral treatment with valganciclovir, a relatively new but potential toxic oral drug, is recommended to prevent further hearing deterioration. In this retrospective cohort study we evaluated the relation between the dose of valganciclovir and the reduction of CMV viral load, as well as the toxicity. All neonates with gestational

盐酸缬更昔洛韦的合成工艺改进

目的盐酸缬更昔洛韦的合成工艺改进。方法以更昔洛韦为原料,经乙酰基保护单羟基制得O-单乙酰更昔洛韦,与Cbz-L-缬氨酸经缩合,再经盐酸脱乙酰基得更昔洛韦-Cbz-L-单缬氨酸酯,酸化后在连续流反应器中催化氢化脱苄氧羰基得盐酸缬更昔洛韦粗品,粗品在异丙醇/水(2:1,V/V)中重结晶得到盐酸缬更昔洛韦。结果工艺改进后的操作更加简便安全,可以实现长时间稳定和安全的连续流生产及后处理,目标产品1的收率和纯度得到提高,总收率48.8%,纯度99.4%。结论为盐酸缬更昔洛韦的合成提供了一种较新的方法,生产成本得以降低。

Management of cytomegalovirus infection after liver transplantation

Cytomegalovirus(CMV)infection is one of the primary causes of morbidity and mortality following liver transplantation(LT).Based on current worldwide guidelines,the most effective strategies for avoiding post-transplant CMV infection are antiviral prophylaxis and pre-emptive treatment.CMV-IgG serology is the established technique for pretransplant screening of both donors and recipients.The clinical presentation of CMV infection and disease exhibits variability,prompting clinicians to consistently consider this possibility,partic-ularly within the first year post-transplantation or subsequent to heightened immunosuppression.At annual symposia to discuss CMV prevention and how treatment outcomes can be improved,evidence on the incorporation of immune functional tests into clinical practice is presented,and the results of studies with new antiviral treatments are evaluated.Although there are ongoing studies on the use of letermovir and maribavir in solid organ transplantation,a consensus reflected in the guidelines has not been formed.Determining the most appro-priate strategy at the individual level appears to be the key to enhancing out-comes.Although prevention strategies reduce the risk of CMV disease,the disease can still occur in up to 50%of high-risk patients.A balance between the risk of infection and disease development and the use of immunosuppressants must be considered when talking about the proper management of CMV in solid organ transplant recipients.The objective of this study was to establish a compre-hensive framework for the management of CMV in patients who have had LT.

Valganciclovir for pre-emptive therapy of cytomegalovirus viraemia after hematopoietic stem cell transplantation： a prospective multi-center trial

Background Despite its widespread use in the management of HIV-related cytomegalovirus （CMV） infection, there have been surprisingly few reports of the use of valganciclovir （VGC） in the post-allotransplant setting.So far, no multi-center, non-crossover trial data have been available with the use of this drug as the primary pre-emptive.The present study evaluated the efficacy and safety of VGC for preemptive therapy of CMV infection after allogeneic hematopoietic stem cell transplantation （HSCT）.Methods From January to April 2007, VGC was adopted in eleven centers in China's Mainland for pre-emptive therapy of CMV infection in consecutive patients undergoing allogeneic HSCT.Allogeneic HSCT recipients were followed weekly via CMV pp65 antigenemia assay or real-time quantitative polymerase chain reaction （PCR） for detection of CMV-DNA.Patients with a positive assay were treated with VGC, 900 mg P.O.twice a day for 14 days followed by 900 mg P.O.once a day for 14 days after a negative result or the CMV-DNA load was lower.Results A total of 54 patients （15 siblings, 28 mismatched related donors, 11 unrelated donors） had a positive assay treated with oral VGC.The seroconversion rate was 89% （48/54） as confirmed by a negative assay; six patients failed oral VGC.No significant toxicity was encountered.No case of CMV disease was diagnosed in the responding patients with a median follow-up of 5.3 months after the drug administration.Conclusion Pre-emptive therapy of CMV viraemia with oral VGC is safe and effective in allogeneic HSCT.

公民逝世后器官捐献供肾移植中巨细胞病毒感染情况及治疗的分析

目的总结公民逝世后器官捐献供肾移植中巨细胞病毒(cytomegalovirus,CMV)感染情况分析及预防、抢先治疗的有效性和安全性。方法回顾分析自2018年1月1日至2021年12月30日在本院首次行公民逝世后器官捐献(deceased donor,DD)异体肾移植243例患者中,挑选符合研究标准的90例患者资料,将其按照CMV病毒载量不同,分为CMV预防治疗组(A组)40例,CMV感染抢先治疗组(B组)34例,无CMV感染证据的阴性对照组(C组)16例,对比观察术后CMV感染特点、与他克莫司(tacrolimus,Tac)谷浓度(C0)相关性、CMV低基质磷酸化蛋白(low matrix phosphoprotein 65,pp65)抗原血症结果与CMV-DNA的一致性以及低剂量缬更昔洛韦(450 mg/d或450 mg/2 d)预防治疗、标准剂量更昔洛韦〔8~10 mg/(kg·d)〕抢先治疗的安全性和有效性等。结果CMV感染在DD肾移植术后总发生率为82.22%(74/90),发生于术后3个月内的比例:A组为90%(36/40),B组94.11%(32/34,χ^(2)=0.0481,P>0.05),使用巴利昔单抗诱导的患者,CMV感染发生时间为(65.62±45.74)d,使用rATG组为(33.06±20.11)d(t=2.9922,P<0.01),Tac的C0与CMV是否感染无相关性(F=0.2879,P>0.05),CMV-pp65抗原血症结果与CMV-DNA的阳性符合率为96.4%,总符合率为65.5%。CMV-pp65抗原血症阳性的样本CD8+T细胞(Ts/Tc)绝对值及NK细胞绝对值均低于pp-65阴性的样本,差异有统计学意义(P<0.05)。低剂量的缬更昔洛韦及标准剂量更昔洛韦用于DD肾移植术后预防及抢先治疗在有效性、不良反应、急性排斥反应(acute rejection,AR)方面对比,差异无统计学意义(P>0.05)。结论低剂量的缬更昔洛韦及标准剂量更昔洛韦用于DD肾移植术后预防及抢先治疗中安全有效。在积极监测术后CMV感染中,CMV-pp65、CD8+T细胞(Ts/Tc)绝对值、NK细胞绝对值能够更及时、准确地帮助诊断CMV感染。

盐酸缬更昔洛韦合成条件的研究

以更昔洛韦为原料,经单乙酰化,缩合,水解,氢化还原四个步骤合成盐酸缬更昔洛韦,并讨论了反应时间,反应温度,投料比例等因素对反应的影响,通过单因素试验和正交试验,改进了反应条件,提高了产率,总收率达到37.62%。

核苷类抗病毒前药的研究进展

一些核苷类抗病毒药物口服给药后,水溶性和口服生物利用度都很差,对这些药物进行修饰,制成其前药的形式,来克服这些不足是非常重要的。该文阐述了近年来核苷类抗病毒前药的设计方法,列举了一些核苷类抗病毒前药并讨论了这些化合物的活性机理。

2种抗病毒药物预防肾移植术后巨细胞病毒肺炎的疗效及安全性探讨

目的评价2种抗病毒药物预防肾移植术后巨细胞病毒(cytomegalovirus,CMV)肺炎的效果和安全性。方法对未使用抗病毒药物或预先应用喷昔洛韦(penciclovir,PCV)或缬更昔洛韦(valganciclovir,VGC)的肾移植受者进行回顾性研究,探讨上述药物对肾移植术后CMV肺炎的预防效果和安全性。结果共82例肾移植受者的临床资料纳入本项研究。术后6个月内,VGC组、PCV组和空白对照组(Sham组)患者CMV肺炎发病率分别为27.5%,18.9%和56.3%,差异有统计学意义(P<0.05),其中VGC组和PCV组间无统计学差异(P>0.05)。治疗12个月后,VGC组、PCV组和Sham组患者CMV肺炎发病率分别为6例(20.6%),5例(13.5%)和3例(18.7%),各组间无统计学差异(P>0.05)。进一步研究发现,治疗6个月后,VGC组、PCV组和Sham组患者重症CMV肺炎发病率分别为13.8%,0和12.5%,其中PCV组重症CMV肺炎发病率较其他2组显著降低(P<0.05)。结论 PCV可以预防肾移植术后CMV肺炎的发生。与VGC相比,PCV对术后早期重症CMV肺炎的预防效果可能更为显著。

液相色谱-串联质谱法测定缬更昔洛韦血药浓度及其在健康人体的药代动力学研究

目的研究缬更昔洛韦片剂(抗病毒药)在健康人体内的原药缬更昔洛韦及其活性代谢产物更昔洛韦的药代动力学过程。方法20名健康男性受试者单次口服缬更昔洛韦片900mg,用LC-MS/MS测定给药后不同时间血浆中缬更昔洛韦及其活性代谢产物更昔洛韦的浓度,研究缬更昔洛韦与更昔洛韦的药代动力学特征。结果主要药代动力学参数如下。缬更昔洛韦:AUC0-t为(606.83±245.53)μg·h·L-1;AUC0-∞为(616.52±247.89)μg·h·L-1;Cmax为(423.56±178.20)μg·L-1;tmax为(1.15±0.41)h;t1/2为(0.82±0.25)h;MRT0-t为(1.58±0.37)h;MRT0-∞为(1.66±0.38)h;Ka为(2.57±2.53)h-1;Ke为(0.91±0.24)h-1;V/F为(1963.85±920.05)L;CL/F为(1688.77±636.77)L·h-1。更昔洛韦:AUC0-t为:(24.99±7.78)mg·h·L-1,AUC0-∞为(26.37±7.80)mg·h·L-1;Cmax为(7.11±1.96)mg·L-1;tmax为(1.76±0.59)h;t1/2为(3.49±0.96)h;MRT0-t为(4.04±0.80)h;MRT0-∞为(4.81±0.84)h;Ka为(1.13±1.20)h-1;Ke为(0.21±0.07)h-1;V/F为(178.55±44.82)L;CL/F为(37.33±11.92)L·h-1。结论本文建立的测定方法,简单、快速、无干扰,适合人体内血药浓度监测和药代动力学研究。

抗病毒药物缬更昔洛韦的合成研究

目的探索更简便的合成缬更昔洛韦的工艺路线,为进一步研究开发提供基础。方法以更昔洛韦为原料,经过酯化、还原两步反应得到目标物缬更昔洛韦。结果实验路线简便,总收率达到20%。结论本文探索了简便的缬更昔洛韦合成工艺,确立了比较合理的酯化条件,改进了氢化脱保护基条件,为将该工艺用于中试放大提供了依据。

先天性巨细胞病毒感染抗病毒治疗的效果和安全性观察

目的观察更昔洛韦(GCV)和(或)缬更昔洛韦(VGCV)治疗先天性巨细胞病毒(CMV)感染患儿的疗效和不良反应。方法回顾性纳入2012年3月1日至2017年5月31日在复旦大学附属儿科医院(我院)新生儿科住院、确诊为先天性CMV感染的患儿,随访至2017年12月31日。从病史资料中提取患儿的一般资料,抗CMV治疗的药物和疗程,新生儿期及1、3和6月龄的肝脾触诊检查结果、胆红素和肝功能检查指标、CMV抗体和DNA检测结果、颅脑MRI、眼底检查结果和听力检测结果,治疗期间药物的不良反应。根据抗病毒治疗与否以及疗程长短分组,比较各组的临床特征和治疗反应。结果 28例先天性CMV感染患儿进入本文分析,其中早产儿11例,男17例;无症状/轻度症状9例,未予抗病毒治疗;中重度症状19例,GCV和(或)VGCV治疗≤6周组11例,治疗6个月组8例。(1)6月龄时,除1例胆汁酸轻度升高外27例中枢神经系统以外的症状和体征、胆红素、肝功能和血常规均恢复正常。(2)无症状/轻度症状组1例在6月龄时出现左侧听力中度损失。治疗≤6周组中,2例CMV相关眼底病变于1月龄时消失;颅脑MRI异常信号和听力损失者各5例,6月龄时分别有3例和2例无改善。治疗6个月组中,4例先天性CMV感染相关视网膜病变在随访中均消失;3例头颅MRI异常信号者和7例有听力损失者,6月龄时分别有2例和1例无改善。(3)治疗≤6周组和治疗6个月组在6月龄时中枢神经系统病变改善情况差异无统计学意义。(4)治疗过程中未发现与GCV和VGCV应用相关的粒细胞减少和肝功能异常。结论抗病毒治疗能改善感音神经性耳聋和脉络膜视网膜炎,GCV和(或)VGCV≤6周与6个月的治疗效果相近;建议对无临床症状先天性CMV感染患儿行眼底检查、脑干诱发电位和头颅MRI检查。

新型抗病毒药物缬更昔洛韦的合成综述

缬更昔洛韦是国际最新抗病毒药物,是更昔洛韦的前体药物,主要用来治疗HIV感染者(AIDS患者)因感染巨细胞病毒(CMV)所致急性视网膜炎。缬更昔洛韦的口服生物利用度比更昔洛韦高出很多,而毒性却大大降低,具有广阔的市场前景,因此综述了缬更昔洛韦的合成方法,并对各种方法进行了比较分析,总结出各自的优缺点。

Cytomegalovirus infection after liver transplantation: Current concepts and challenges

Cytomegalovirus (CMV) is a common viral pathogen that influences the outcome of liver transplantation. In addition to the direct effects of CMV syndrome and tissue-invasive diseases, CMV is associated with an increased predisposition to acute and chronic allograft rejection, accelerated hepatitis C recurrence, and other opportunistic infections, as well as reduced overall patient and allograft survival. Risk factors for CMV disease are often interrelated, and include CMV D+/R-serostatus, acute rejection, female gender, age, use of high-dose mycophenolate mofetil and prednisone, and the overall state of immunity. In addition to the role of CMV-specif ic CD4+ and CD8+ T lymphocytes, there are data to suggest that functionality of the innate immune system contributes to CMV disease pathogenesis. In one study, liver transplant recipients with a specific polymorphism in innate immune molecules known as Toll-like receptors were more likely to develop higher levels of CMV replication and clinical disease. Because of the direct and indirect adverse effects of CMV disease, its prevention, whether through antiviral prophylaxis or preemptive therapy, is an essential component in improving the outcome of liver transplantation. In the majority of transplant centers, antiviral prophylaxis is the preferred strategy over preemptive therapy for the prevention of CMV disease in CMV-seronegative recipients of liver allografts from CMV-seropositive donors (D+/R-). However, the major drawback of antiviral prophylaxis is the occurrence of delayed-onset primary CMV disease. In several prospective and retrospective studies, the incidence of delayed-onset primary CMV disease ranged from 16% to 47% of CMV D+/R-liver transplant recipients.Current data suggests that delayed-onset CMV disease is associated with increased mortality after liver transplantation. Therefore, optimized strategies for prevention and novel drugs with unique modes of action are needed. Currently, a randomized controlled clinical trial is being performed comparing the effi cacy and safety of maribavir, a novel benzimidazole riboside, and oral ganciclovir as prophylaxis against primary CMV disease in liver transplant recipients. The treatment of CMV disease consists mainly of intravenous (IV) ganciclovir, and if feasible, a reduction in the degree of immunosuppression. A recent controlled clinical trial demonstrated that valganciclovir is as effective and safe as IV ganciclovir for the treatment of CMV disease in solid organ (including liver) transplant recipients. In this article, the author reviews the current state and the future perspectives of prevention and treatment of CMV disease after liver transplantation.

口服抗病毒新药——缬更昔洛韦

缬更昔洛韦 (valganciclovir)是抗病毒药更昔洛韦的前体药物 ,用于治疗AIDS病人发生的巨细胞病毒 (CMV)视网膜炎。缬更昔洛韦口服后迅速吸收 ,并水解为更昔洛韦 ,其口服给药的生物利用度较高 (60 % )。试验表明 ,口服缬更昔洛韦 (90 0mg)与静脉注射更昔洛韦 (5mg·kg-1) ,bid,3wk后改为 qd ,治疗 1 60例AIDS病人发生的CMV视网膜炎有相同疗效 ,且耐受性相似。缬更昔洛韦维持治疗中最常见的不良反应为中性粒细胞减少症、贫血、胃肠道反应 (腹泻、恶心、呕吐 )、发热。

Two strategies for prevention of cytomegalovirus infections after liver transplantation

AIM: To analyze differences in patients' clinical course, we compared two regimes of either preemptive therapy or prophylaxis after liver transplantation.METHODS: This retrospective study was reviewed and approved by the institutional review board of the University of Leipzig. Cytomegalovirus(CMV) prophylaxis with valganciclovir hydrochloride for liver transplant recipients was replaced by a preemptive strategy in October 2009. We retrospectively compared liver transplant recipients 2 years before and after October 2009. During the first period, all patients received valganciclovir daily. During the second period all patients included in the analysis were treated following a preemptive strategy. Outcomes included one year survival and therapeutic intervention due to CMV viremia or infection.RESULTS: Between 2007 and 2010 n = 226 patients underwent liver transplantation in our center. n = 55 patients were D^+/R^- high risk recipients and were excluded from further analysis. A further 43 patients had to be excluded since CMV prophylaxis/preemptive strategy was not followed although there was no clinical reason for the deviation. Of the remaining 128 patients whose data were analyzed, 60 receivedprophylaxis and 68 were treated following a preemptive strategy. The difference in overall mortality was not significant, nor was it significant for one-year mortality where it was 10%(95%CI: 8%-28%, P = 0.31) higher for the preemptive group. No significant differences in blood count abnormalities or the incidence of sepsis and infections were observed other than CMV. In total, 19 patients(14.7%) received ganciclovir due to CMV viremia and/or infections. Patients who were treated according to the preemptive algorithm had a significantly higher rate risk of therapeutic intervention with ganciclovir [n = 16(23.5%) vs n = 3(4.9%), P = 0.003)].CONCLUSION: These data suggest that CMV prophylaxis is superior to a preemptive strategy in patients undergoing liver transplantation.

Current concepts on cytomegalovirus infection after liver transplantation

Cytomegalovirus (CMV) is the most common viral pa- thogen that negatively impacts on the outcome of liver transplantation. CMV cause febrile illness often ac com panied by bone marrow suppression, and in some cases, invades tissues including the transplanted allog raft. In addition, CMV has been signif icantly asso- ciated with an increased predisposition to allograft re- jection, accelerated hepatitis C recurrence, and other opportunistic infections, as well as reduced overall pa tient and allograft survival. To negate the adverse effects of CMV on outcome, its prevention, whether through antiviral prophylaxis or preemptive therapy, is regarded as an essential component to the medical management of liver transplant patients. Two recent guidelines have suggested that antiviral prophylaxis or preemptive therapy are similarly effective in preventing CMV disease in modest-risk CMV-seropositive liver trans plant recipients, while antiviral prophylaxis is the preferred strategy over preemptive therapy for the preven tion of CMV disease in high-risk recipients [CMV-ser o-negative recipients of liver allografts from CMV-seropositive donors (D+/R-)]. However, antiviral prophylax is has only delayed the onset of CMV disease in many CMV D+/R- liver transplant recipients, and at least in one study, such occurrence of late-onset primary CMV disease was significantly associated with increased mortality after liver transplantation. Therefore, optimized strategies for prevention are needed, and aggressive treatment of CMV infection and disease should be pursued. The standard treatment of CMV disease consists of intravenous ganciclovir or oral valganciclovir, and if fea sible, one should also reduce the degree of immuno-suppression. In one recent controlled clinical trial, val ganc iclovir was found to be as effective and safe as intravenous ganciclovir for the treatment of mild to mo d erate CMV disease in solid organ (including liver) tran splant recipients. In this article, the authors review the current state and the future perspectives of prev ention and treatment of CMV disease after liver trans plantation.

Management of cytomegalovirus infection and disease in liver transplant recipients

Cytomegalovirus(CMV) is one of the most common viral pathogens causing clinical disease in liver transplant recipients, and contributing to substantial morbidity and occasional mortality. CMV causes febrile illness often accompanied by bone marrow suppression, and in some cases, invades tissues including the transplanted liver allograft. In addition, CMV has been significantly associated with an increased predisposition to acute and chronic allograft rejection, accelerated hepatitis C recurrence, and other opportunistic infections, as well as reduced overall patient and allograft survival. To negate the adverse effects of CMV infection on transplant outcome, its prevention, whether through antiviral prophylaxis or preemptive therapy, is an essential component to the management of liver transplant recipients. Two recently updated guidelines have suggested that antiviral prophylaxis or preemptive therapy are similarly effective in preventing CMV disease in modest-risk CMV-seropositive liver transplant recipients, while antiviral prophylaxis is the preferredstrategy over preemptive therapy for the prevention of CMV disease in high-risk recipients [CMV-seronegative recipients of liver allografts from CMV-seropositive donors(D+/R-)]. However, antiviral prophylaxis has only delayed the onset of CMV disease in many CMV D+/Rliver transplant recipients, and such occurrence of lateonset CMV disease was significantly associated with increased all-cause and infection-related mortality after liver transplantation. Therefore, a search for better strategies for prevention, such as prolonged duration of antiviral prophylaxis, a hybrid approach(antiviral prophylaxis followed by preemptive therapy), or the use of immunologic measures to guide antiviral prophylaxis has been suggested to prevent late-onset CMV disease. The standard treatment of CMV disease consists of intravenous ganciclovir or oral valganciclovir, and if feasible, reduction in pharmacologic immunosuppression. In one clinical trial, oral valganciclovir was as effective as intravenous ganciclovir for the treatment of mild to moderate CMV disease in solid organ(including liver) transplant recipients. The aim of this article is to provide a state-of-the art review of the epidemiology, diagnosis, prevention, and treatment of CMV infection and disease after liver transplantation.

Cytomegalovirus infection in liver transplant recipients: Updates on clinical management

Cytomegalovirus(CMV) infection is a common complication after liver transplantation, and it is associated with multiple direct and indirect effects. Management of CMV infection and disease has evolved over the years,and clinical guidelines have been recently updated.Universal antiviral prophylaxis and a pre-emptive treatment strategy are options for prevention. A currentlyrecruiting randomized clinical trial is comparing the efficacy and safety of the two prevention strategies in the highest risk D+R- liver recipients. Drug-resistant CMV infection remains uncommon but is now increasing in incidence. This highlights the currently limited therapeutic options, and the need for novel drug discoveries.Immunotherapy and antiviral drugs with novel mechanisms of action are being investigated, including letermovir(AIC246) and brincidofovir(CMX001). This article reviews the current state of CMV management after liver transplantation, including the updated practice guidelines, and summarizes the data on investigational drugs and vaccines in clinical development.

口服缬更昔洛韦治疗新生儿先天性巨细胞病毒感染1例

目的:探讨口服缬更昔洛韦治疗先天性巨细胞病毒感染新生儿的疗效。方法:口服缬更昔洛韦16 mg/kg,每日2次,治疗1例先天性巨细胞病毒感染新生儿6周,监测新生儿体质量、头围、中性粒细胞、血小板、直接胆红素、丙氨酸氨基转移酶及病毒载量,随访头颅超声、脑干听性诱发电位和头颅磁共振成像(MRI)。结果:缬更昔洛韦治疗后尿液中和血液中病毒载量转阴,听力和发育结果改善,患儿治疗期间出现粒细胞减少症,治疗结束后好转。结论:口服缬更昔洛韦治疗先天性巨细胞病毒感染疗效较显著,需进一步研究确定最佳剂量、疗程以达到更好的疗效和安全性。