Your search keyword '"Cidofovir pharmacology"' showing total 37 results

1. Uncovering the Potent Antiviral Activity of the Sesterterpenoids from the Sponge Ircinia Felix Against Human Adenoviruses: from the Natural Source to the Total Synthesis.

Author

Ruiz-Molina A, Pech-Puch D, Millán RE, Ageitos L, Villegas-Hernández H, Pachón J, Pérez Sestelo J, Sánchez-Céspedes J, Rodríguez J, and Jiménez C

Subjects

Humans, Animals, Structure-Activity Relationship, Lactams chemistry, Lactams pharmacology, Cidofovir chemistry, Cidofovir pharmacology, Antiviral Agents pharmacology, Antiviral Agents chemistry, Antiviral Agents chemical synthesis, Porifera chemistry, Adenoviruses, Human drug effects, Sesterterpenes chemistry, Sesterterpenes pharmacology, Sesterterpenes chemical synthesis

Abstract

Human Adenovirus (HAdV) infections in immunocompromised patients can result in disseminated diseases with high morbidity and mortality rates due to the absence of available treatments for these infections. The sponge Ircinia felix was selected for the significant anti-HAdV activity displayed by its organic extracts. Its chemical analysis yielded three novel sesterterpene lactams, ircinialactams J-L, along with three known sesterterpene furans which structures were established by a deep spectrometric analysis. Ircinialactam J displayed significant antiviral activity against HAdV without significant cytotoxicity, showing an effectiveness 11 times greater than that of the standard treatment, cidofovir®. Comparison of the antiviral evaluation results of the isolated compounds allowed us to deduce some structure-activity relationships. Mechanistic assays suggest that ircinialactam J targets an early step of the HAdV replicative cycle before HAdV genome reaches the nucleus of the host cell. The first total synthesis of ircinialactam J was also accomplished to prove the structure and to provide access to analogues. Key steps are a regio- and stereoselective construction of the trisubstituted Z-olefin at Δ 7 by iron-catalyzed carbometallation of a homopropargylic alcohol, a stereoselective methylation to generate the stereogenic center at C18, and the formation of the (Z)-Δ 20 by stereoselective aldol condensation to introduce the tetronic acid unit. Ircinialactam J is a promising chemical lead to new potent antiviral drugs against HAdV infections., (© 2024 The Author(s). Chemistry - A European Journal published by Wiley-VCH GmbH.)

Published

2024

2. Treatment efficacy of cidofovir and brincidofovir against clade II Monkeypox virus isolates.

Author

Prévost J, Sloan A, Deschambault Y, Tailor N, Tierney K, Azaransky K, Kammanadiminti S, Barker D, Kodihalli S, and Safronetz D

Subjects

Animals, Mice, Female, Chlorocebus aethiops, Humans, Treatment Outcome, Vero Cells, Virus Replication drug effects, Disease Models, Animal, Mice, Inbred BALB C, Cytosine analogs & derivatives, Cytosine therapeutic use, Cytosine pharmacology, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Cidofovir therapeutic use, Cidofovir pharmacology, Organophosphonates therapeutic use, Organophosphonates pharmacology, Monkeypox virus drug effects, Mpox (monkeypox) drug therapy, Mpox (monkeypox) virology

Abstract

While historically confined to endemic areas, Monkeypox virus (MPXV) infection has increasingly garnered international attention due to sporadic outbreaks in non-endemic countries in the last two decades and its potential for human-to-human transmission. In 2022, a multi-country outbreak of mpox disease was declared by the World Health Organization (WHO) and nearly 100 000 mpox cases have been reported since the beginning of this pandemic. The clade II variant of the virus appears to be responsible for the vast majority of these infections. While there are no antiviral drugs currently approved to treat mpox specifically, the use of tecovirimat (TPOXX®) and brincidofovir (Tembexa®) is recommended by the Centers for Disease Control and Prevention (CDC) for compassionate use in severe mpox cases, since both are FDA-approved for the treatment of the closely related smallpox disease. Given the emergence of multiple tecovirimat-resistant infections, we aimed to evaluate the treatment efficacy of brincidofovir and its active compound, cidofovir, against MPXV clade II strains. Following intranasal infection, we show that cidofovir and brincidofovir can strongly reduce the viral replication of MPXV clade IIa and IIb viruses in the respiratory tract of susceptible mice when administered systemically and orally, respectively. The high antiviral activity of both compounds against historical and currently circulating MPXV strains supports their therapeutic potential for clinical application., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Srinivas Kammanadiminti reports a relationship with Emergent BioSolutions Inc that includes: employment. Douglas Barker reports a relationship with Emergent BioSolutions Inc that includes: employment. Shantha Kodihalli reports a relationship with Emergent BioSolutions Inc that includes: employment. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Crown Copyright © 2024. Published by Elsevier B.V. All rights reserved.)

Published

2024

3. Combined Effect of Basic Antiherpetic Drugs with a New Inhibitor of the Terminase Complex of Herpes Simplex Virus Type 1 in Vero Cell Cultures.

Author

Andronova VL, Galegov GA, Vozdvizhenskaya OA, Levit GL, Krasnov VP, and Charushin VN

Subjects

Vero Cells, Chlorocebus aethiops, Animals, Ganciclovir pharmacology, Foscarnet pharmacology, Guanine analogs & derivatives, Guanine pharmacology, Cidofovir pharmacology, Humans, Bromodeoxyuridine analogs & derivatives, Antiviral Agents pharmacology, Herpesvirus 1, Human drug effects, Herpesvirus 1, Human physiology, Endodeoxyribonucleases metabolism, Endodeoxyribonucleases antagonists & inhibitors, Acyclovir pharmacology

Abstract

Carriers of herpes simplex virus type 1 (HSV-1) account for more than 90% of the global population. Infection manifests itself in the formation of blisters and ulcers on the face or genitals and can cause blindness, encephalitis, and generalized infection. All first- and second-line modern antiherpetic drugs selectively inhibit viral DNA polymerase. The purine-benzoxazine conjugate LAS-131 ((S)-4-[6-(purin-6-yl)aminohexanoyl]-7,8-difluoro-3,4-dihydro-3-methyl-2H-[1,4]benzoxazine), which we have described earlier, uses the large subunit of the HSV-1 terminase complex as a biotarget and selectively inhibits HSV-1 reproduction in vitro. Basically new results were for the first time obtained to characterize the combined effect on human herpesvirus infection for LAS-131 used in combination with practically significant antiviral compounds, including the nucleoside analogs acyclovir (ACV), penciclovir (PCV), ganciclovir (GCV), brivudine (BVdU), iododeoxyuridine (IdU), and adenine arabinoside (Ara-A); the nucleoside phosphonate analog cidofovir (CDV); and the pyrophosphate analog foscarnet (FOS). A cytopathic effect (CPE) inhibition assay showed that the drug concentration that inhibited the virus-induced CPE by 50% decreased by a factor of 2 (an additive effect, FOS) or more (a synergistic effect; ACV, PCV, GCV, IdU, BVdU, Ara-A, and CDV) when the drugs were used in combination with LAS-131. Nonpermissive conditions for HSV-1 reproduction were thus created at lower drug concentrations, opening up new real possibilities to control human herpesvirus infection., (© 2024. Pleiades Publishing, Ltd.)

Published

2024

4. NPP-669, a prodrug of cidofovir, is highly efficacious against human adenovirus infection in the permissive Syrian hamster model.

Author

Tollefson AE, Cline-Smith AB, Spencer JF, Reyna DM, Lipka E, and Toth K

Subjects

Animals, Humans, Adenoviruses, Human drug effects, Adenovirus Infections, Human drug therapy, Adenovirus Infections, Human virology, Disease Models, Animal, Cricetinae, Administration, Oral, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Prodrugs pharmacology, Prodrugs therapeutic use, Cidofovir pharmacology, Cidofovir therapeutic use, Mesocricetus, Organophosphonates pharmacology, Organophosphonates therapeutic use, Cytosine analogs & derivatives, Cytosine pharmacology, Cytosine therapeutic use

Abstract

Human adenoviruses can cause serious, disseminated infections in immunocompromised patients. For pediatric allogeneic stem cell transplant patients, the case fatality rate can reach 80%. Still, there is no available antiviral drug that is specifically approved by the Food and Drug Administration for the treatment of adenovirus infections. To fill this pressing medical need, we have developed NPP-669, a prodrug of cidofovir with broad activity against double-stranded DNA viruses, including adenoviruses. Here, we report on the in vivo anti-adenoviral efficacy of NPP-669. Using the immunosuppressed Syrian hamster as the model, we show that NPP-669 is highly efficacious when dosed orally at 1 mg/kg and 3 mg/kg. In a delayed administration experiment, NPP-669 was more effective than brincidofovir, a similar compound that reached Phase III clinical trials. Furthermore, parenteral administration of NPP-669 increased its efficacy approximately 10-fold compared to oral dosing without apparent toxicity, suggesting that this route may be preferable in a hospital setting. Based on these findings, we believe that NPP-669 is a promising new compound that needs to be further investigated., Competing Interests: The authors declare no conflict of interest.

Published

2024

5. Structural basis of human mpox viral DNA replication inhibition by brincidofovir and cidofovir.

Author

Xu Y, Wu Y, Wu X, Zhang Y, Yang Y, Li D, Yang B, Gao K, Zhang Z, and Dong C

Subjects

Humans, DNA, Viral, Models, Molecular, Mpox (monkeypox), Cidofovir pharmacology, Cidofovir chemistry, Organophosphonates pharmacology, Organophosphonates chemistry, Cytosine analogs & derivatives, Cytosine pharmacology, Cytosine chemistry, DNA Replication drug effects, Antiviral Agents pharmacology, Antiviral Agents chemistry, Virus Replication drug effects

Abstract

Mpox virus has wildly spread over 108 non-endemic regions in the world since May 2022. DNA replication of mpox is performed by DNA polymerase machinery F8-A22-E4, which is known as a great drug target. Brincidofovir and cidofovir are reported to have broad-spectrum antiviral activity against poxviruses, including mpox virus in animal models. However, the molecular mechanism is not understood. Here we report cryogenic electron microscopy structures of mpox viral F8-A22-E4 in complex with a DNA duplex, or dCTP and the DNA duplex, or cidofovir diphosphate and the DNA duplex at resolution of 3.22, 2.98 and 2.79 Å, respectively. Our structural work and DNA replication inhibition assays reveal that cidofovir diphosphate is located at the dCTP binding position with a different conformation to compete with dCTP to incorporate into the DNA and inhibit DNA synthesis. Conformation of both F8-A22-E4 and DNA is changed from the pre-dNTP binding state to DNA synthesizing state after dCTP or cidofovir diphosphate is bound, suggesting a coupling mechanism. This work provides the structural basis of DNA synthesis inhibition by brincidofovir and cidofovir, providing a rational strategy for new therapeutical development for mpox virus and other pox viruses., Competing Interests: Declaration of competing interest The authors declare that there is no conflict of interest., (Copyright © 2024. Published by Elsevier B.V.)

Published

2024

6. Oral USC-093, a novel homoserinamide analogue of the tyrosinamide (S)-HPMPA prodrug USC-087 has decreased nephrotoxicity while maintaining antiviral efficacy against human adenovirus infection of Syrian hamsters.

Author

Tollefson AE, Riemann SB, Ying B, Spencer JF, Overhulse JM, Kashemirov BA, Wold WSM, McKenna CE, and Toth K

Subjects

Cricetinae, Animals, Humans, Cidofovir pharmacology, Cidofovir therapeutic use, Mesocricetus, Antiviral Agents therapeutic use, Adenoviridae, Virus Replication, Cytosine pharmacology, Cytosine therapeutic use, Amino Acids pharmacology, Nucleotides therapeutic use, Adenovirus Infections, Human drug therapy, Prodrugs pharmacology, Prodrugs therapeutic use, Organophosphonates pharmacology, Organophosphonates therapeutic use, Adenoviridae Infections drug therapy, Adenine analogs & derivatives, Tyrosine analogs & derivatives

Abstract

Adenovirus infections of immunocompromised humans are a significant source of morbidity and mortality. Presently, there is no drug specifically approved for the treatment of adenovirus infections by the FDA. The state-of-the-art treatment of such infections is the off-label use of cidofovir, an acyclic nucleotide phosphonate. While cidofovir inhibits adenovirus replication, it has dose-limiting kidney toxicity. There is an apparent need for a better compound to treat adenovirus infections. To this end, we have been developing acyclic nucleotide phosphonate prodrugs that utilize an amino acid scaffold equipped with a lipophilic modifier. Here, we compare the antiviral potential of two prodrugs of HPMPA that differ only in the amino acid-based promoiety: USC-087, based on an N-hexadecyl tyrosinamide, and USC-093, based on an N-hexadecyl serinamide. Oral administration of both compounds was very efficacious against disseminated HAdV-C6 infection in immunosuppressed Syrian hamsters, suppressing virus replication and mitigating pathology even when treatment was withheld until 4 days after challenge. We saw only marginal efficacy after respiratory infection of hamsters, which may reflect suboptimal distribution to the lung. Importantly, neither compound induced intestinal toxicity, which was observed as the major adverse effect in clinical trials of brincidofovir, a prodrug of cidofovir which also contains a C-16 modifier. Notably, we found that there was a significant difference in the nephrotoxicity of the two compounds: USC-087 caused significant kidney toxicity while USC-093 did not, at effective doses. These findings will be valuable guidepoints in the future evolution of this new class of potential prodrugs to treat adenovirus infections., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

7. Therapeutic strategies against BK polyomavirus infection in kidney transplant recipients: Systematic review and meta-analysis.

Author

Zhong C, Chen J, Yan Z, Xia R, Zeng W, Deng W, Xu J, Wang Y, and Miao Y

Subjects

Humans, Cidofovir pharmacology, Cidofovir therapeutic use, Leflunomide therapeutic use, Leflunomide pharmacology, Immunoglobulins, Intravenous therapeutic use, Transplant Recipients, Kidney Transplantation adverse effects, Polyomavirus Infections drug therapy, BK Virus, Tumor Virus Infections drug therapy

Abstract

Background: The selection of antiviral therapy for BK polyomavirus (BKPyV) infection has been extensively debated. Our study aimed to assess the efficacy and safety of various treatments for BKPyV infection., Methods: We searched PubMed, EMBASE, and Web of Science databases for relevant studies regarding drug treatments for BKPyV viremia/DNAemia published between January 1, 1970 and September 30, 2022. Two independent authors screened the published studies, extracted pertinent data, and evaluated their methodological quality. A meta-analysis was performed using the RevMan software version 4.2.2., Results: A total of 33 published studies involving 986 patients were included in the meta-analysis. Overall, therapeutic interventions comprised immunosuppression reduction alone or in combination with leflunomide, intravenous immunoglobulin (IVIG), cidofovir, or mTOR inhibitor (mTORi) therapy. The meta-analysis revealed that the efficacy of immunosuppression reduction alone for serum BKPyV clearance was 68% (95% confidence interval [CI]: 0.58-0.77; I 2  = 78%). Moreover, the efficacy of immunosuppression reduction in combination with leflunomide, cidofovir, IVIG, or mTORi therapy for serum BKPyV clearance was 61% (95% CI: 0.47-0.74; I 2  = 83%), 71% (95% CI: 0.63-0.78; I 2  = 0), 87% (95% CI: 0.82-0.93; I 2  = 45%), and 80% (95% CI: 0.59-1.00; I 2  = 58%), respectively. Compared to immunosuppression reduction alone, immunosuppression reduction combined with IVIG therapy offered a statistically significant benefit in serum BKPyV clearance (P < 0.01) with minimal adverse reactions, whereas other adjunctive drug treatments did not demonstrate considerable effects., Conclusions: Reducing immunosuppression remains the primary approach for treating BKPyV infection. Although the combination treatment with IVIG proved to be most effective, other agents might offer varied antiviral advantages of high heterogeneity, which should be substantiated in future long-term randomized controlled trials., Competing Interests: Declaration of Competing Interest None., (Copyright © 2023 Elsevier B.V. All rights reserved.)

Published

2023

8. Disulfide-incorporated lipid prodrugs of cidofovir: Synthesis, antiviral activity, and release mechanism.

Author

Wang B, Cao B, Bei ZC, Xu L, Zhang D, Zhao L, Song Y, and Wang H

Subjects

Animals, Chlorocebus aethiops, Humans, Cidofovir pharmacology, Vero Cells, Micelles, Cytosine pharmacology, Cytosine chemistry, Vaccinia virus, Lipids, Phosphates, Mpox (monkeypox), Antiviral Agents chemistry, Prodrugs pharmacology

Abstract

The double-stranded DNA (dsDNA) viruses represented by adenovirus and monkeypox virus, have attracted widespread attention due to their high infectivity. In 2022, the global outbreak of mpox (or monkeypox) has led to the declaration of a Public Health Emergency of International Concern. However, to date therapeutics approved for dsDNA virus infections remain limited and there are still no available treatments for some of these diseases. The development of new therapies for treating dsDNA infection is in urgent need. In this study, we designed and synthesized a series of novel disulfide-incorporated lipid conjugates of cidofovir (CDV) as potential candidates against dsDNA viruses including vaccinia virus (VACV) and adenovirus (AdV) 5. The structure-activity relationship analyses revealed that the optimum linker moiety was C 2 H 4 and the optimum aliphatic chain length was 18 or 20 atoms. Among the synthesized conjugates, 1c exhibited more potency against VACV (IC 50  = 0.0960 μM in Vero cells; IC 50  = 0.0790 μM in A549 cells) and AdV5 (IC 50  = 0.1572 μM in A549 cells) than brincidofovir (BCV). The transmission electron microscopy (TEM) images revealed that the conjugates could form micelles in phosphate buffer. The stability studies in the GSH environment demonstrated that the formation of micelles in phosphate buffer might protect the disulfide bond from glutathione (GSH) reduction. The dominant means of the synthetic conjugates to liberate the parent drug CDV was by enzymatic hydrolysis. Furthermore, the synthetic conjugates remained sufficiently stable in simulated gastric fluid (SGF), simulated intestinal fluid (SIF), and pooled human plasma, which indicated the possibility for oral administration. These results indicated 1c may be a broad-spectrum antiviral candidate against dsDNA viruses with potential oral administration. Moreover, modification of the aliphatic chain attached to the nucleoside phosphonate group was involved as an efficient prodrug strategy for the development of potent antiviral candidates., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 Elsevier Masson SAS. All rights reserved.)

Published

2023

9. Monkeypox: Virology, laboratory diagnosis and therapeutic approach.

Author

Siami H, Asghari A, and Parsamanesh N

Subjects

United States, Humans, Cidofovir pharmacology, Cidofovir therapeutic use, Vaccinia virus genetics, Monkeypox virus genetics, Clinical Laboratory Techniques, Mpox (monkeypox) diagnosis, Mpox (monkeypox) drug therapy, Mpox (monkeypox) epidemiology

Abstract

Monkeypox infection outbreaks have been observed sporadically in Africa, usually as a result of interaction with wildlife reservoirs. The genomes of the new strain range in size from 184.7 to 198.0 kb and are identified with 143-214 open reading frames. Viral cores are rapidly carried on microtubules away from the cell's perimeter and deeper into the cytoplasm once the virus and cell membranes fuse. Depending on the kind of exposure, patients with monkeypox may experience a febrile prodrome 5-13 days after exposure, which frequently includes lymphadenopathy, malaise, headaches, and muscle aches. A different diagnostic approach is available for monkeypox, including histopathological analysis, electron microscopy, immunoassays, polymerase chain reaction, genome sequencing, microarrays, loop-mediated isothermal amplification technology and CRISPR (i.e., "clustered regularly interspaced short palindromic repeats"). There are currently no particular, clinically effective treatments available for the monkeypox virus. An initial treatment is cidofovir. As a monophosphate nucleotide analog, cidofovir is transformed into an inhibitor of viral DNA polymerase by cellular kinases, which is analogous to cidofovir's function in inhibiting viral DNA synthesis. The European Medicine Agency and the Food and Drug Administration have both granted permission for IMVAMUNE, a replication-deficient, attenuated third-generation modified vaccinia Ankara vaccine, to be used for the prevention of smallpox and monkeypox in adults., (© 2023 John Wiley & Sons Ltd.)

Published

2023

10. In Vitro efficacy of cyclosporine a and various antiseptics and antiviral drugs on adenovirus genotype 8, a common cause of epidemic keratoconjunctivitis.

Author

Aydamirov AS, Harbiyeli II, Ozturk G, Yarkin F, Erdem E, and Yagmur M

Subjects

Humans, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Cyclosporine pharmacology, Cyclosporine therapeutic use, Povidone-Iodine pharmacology, Povidone-Iodine therapeutic use, Adenoviridae, Cidofovir pharmacology, Cidofovir therapeutic use, Chlorhexidine pharmacology, Chlorhexidine therapeutic use, Ganciclovir pharmacology, Genotype, Anti-Infective Agents, Local pharmacology, Anti-Infective Agents, Local therapeutic use, Adenoviridae Infections drug therapy, Keratoconjunctivitis drug therapy

Abstract

Purpose: To evaluate the in vitro efficacy of cidofovir, ganciclovir, povidone-iodine, chlorhexidine, and cyclosporine A on adenovirus genotype 8., Methods: Conjunctival samples were collected from patients with adenoviral conjunctivitis and cultured in A549 cells. Adenovirus diagnosis was confirmed by RT-PCR. For each drug, the 50% cytotoxic concentration (CC 50 ) was determined. Subsequently, the antiviral activity was tested at concentrations below CC 50, and the 50% inhibitor concentration (IC 50 ) of drugs was determined RESULTS: While the IC 50 of cidofovir against adenovirus genotype 8 was 3.07 ± 0.8 µM, ganciclovir, povidone-iodine, chlorhexidine, and cyclosporine A were not found to be effective against adenovirus genotype 8 at concentrations below the CC 50 value., Conclusions: Cidofovir was found effective and the IC 50 value was within the ranges in the literature. Ganciclovir and cyclosporine A were found to be ineffective at doses below the cytotoxic dose, povidone-iodine and chlorhexidine was found to be highly cytotoxic., (© 2022. The Author(s), under exclusive licence to Springer Nature B.V.)

Published

2023

11. Arabinofuranosyl Thymine Derivatives-Potential Candidates against Cowpox Virus: A Computational Screening Study.

Author

Haj Hasan A, Preet G, Milne BF, Ebel R, and Jaspars M

Subjects

Animals, Humans, Thymine metabolism, Cidofovir pharmacology, Ligands, Molecular Docking Simulation, Rodentia, Cowpox virus genetics, Cowpox virus metabolism, Cowpox

Abstract

Cowpox is caused by a DNA virus known as the cowpox virus (CPXV) belonging to the Orthopoxvirus genus in the family Poxviridae. Cowpox is a zoonotic disease with the broadest host range among the known poxviruses. The natural reservoir hosts of CPXV are wild rodents. Recently, the cases of orthopoxviral infections have been increasing worldwide, and cowpox is considered the most common orthopoxviral infection in Europe. Cowpox is often a self-limiting disease, although cidofovir or anti-vaccinia gammaglobulin can be used in severe and disseminated cases of human cowpox. In this computational study, a molecular docking analysis of thymine- and arabinofuranosyl-thymine-related structures ( 1-21 ) on two cowpox-encoded proteins was performed with respect to the cidofovir standard and a 3D ligand-based pharmacophore model was generated. Three chemical structures (PubChem IDs: 123370001, 154137224, and 90413364) were identified as potential candidates for anti-cowpox agents. Further studies combining in vitro and in silico molecular dynamics simulations to test the stability of these promising compounds could effectively improve the future design of cowpox virus inhibitors, as molecular docking studies are not sufficient to consider a ligand a potential drug.

Published

2023

12. Amplifying the impact of kidney microphysiological systems: predicting renal drug clearance using mechanistic modelling based on reconstructed drug secretion.

Author

Caetano-Pinto P, Nordell P, Nieskens T, Haughan K, Fenner KS, and Stahl SH

Subjects

Animals, Humans, Cidofovir pharmacology, Kidney metabolism, Drug Elimination Routes, Microphysiological Systems, Metformin metabolism, Metformin pharmacology

Abstract

Accurate prediction of pharmacokinetic parameters, such as renal clearance, is fundamental to the development of effective and safe new treatments for patients. However, conventional renal models have a limited ability to predict renal drug secretion, a process that is dependent on transporters in the proximal tubule. Improvements in microphysiological systems (MPS) have extended our in vitro capabilities to predict pharmacokinetic parameters. In this study a kidney-MPS model was developed that successfully recreated renal drug secretion. Human proximal tubule cells grown in the kidney-MPS, resem­bling an in vivo phenotype, actively secreted the organic cation drug metformin and organic anion drug cidofovir, in contrast to cells cultured in conventional culture formats. Metformin and cidofovir renal secretory clearance were predicted from kid­ney-MPS data within 3.3- and 1.3-fold, respectively, of clinically reported values by employing a semi-mechanistic drug distribution model using kidney-MPS drug transport parameters together with in vitro to in vivo extrapolation. This approach introduces an effective application of a kidney-MPS model coupled with pharmacokinetic modelling tools to evaluate and predict renal drug clearance in humans. Kidney-MPS renal clearance predictions can potentially complement pharma-cokinetic animal studies and contribute to the reduction of pre-clinical species use during drug development.

Published

2023

13. Daily low dose intravesical cidofovir for the treatment of BK virus associated hemorrhagic cystitis after allogeneic stem cell transplantation.

Author

Uzay A, Gündoğdu Y, Koşan B, Yetiş T, Gür H, Okuturlar Y, and Kartı SS

Subjects

Humans, Cidofovir therapeutic use, Cidofovir pharmacology, Cytosine adverse effects, Antiviral Agents adverse effects, Hemorrhage drug therapy, Hemorrhage etiology, BK Virus, Polyomavirus Infections drug therapy, Tumor Virus Infections drug therapy, Organophosphonates adverse effects, Cystitis drug therapy, Cystitis etiology, Hematopoietic Stem Cell Transplantation adverse effects, Hematopoietic Stem Cell Transplantation methods, Drug-Related Side Effects and Adverse Reactions etiology, Renal Insufficiency etiology

Abstract

Introduction: BK virus associated hemorrhagic cystitis(BKV-AHC) is a serious complication observed after allogeneic stem cell transplantation and the current therapeutic options are scarce with substantial renal side effects. Although the guidelines recommend intravenous cidofovir application with caution to nephrotoxicity, there are few studies which investigated intravesical administration and reported similar therapeutic results with less renal side effects., Methods: We administered low dose, daily and consecutive (75 mg/day, for 5 days) intravesical cidofovir to 25 patients with BKV-AHC that developed after (ASCT)., Results: The response rate in our cohort was 92% and relapse was not encountered in 84% of the patient population during one year of follow-up. The median BK urine viral load significantly decreased from 260,000,000 IU/mL to 53,000,000 IU/mL after a week of treatment (p = 0.0001). Rise in serum creatinine was observed in 5 patients during treatment and post-treatment nephrotoxicity was seen in only 1 patient., Conclusions: Daily low dose intravesical cidofovir might be an effective treatment option for BKV-AHC after ASCT with favorable less systemic side effects., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 Japanese Society of Chemotherapy and The Japanese Association for Infectious Diseases. Published by Elsevier Ltd. All rights reserved.)

Published

2023

14. Filociclovir is a potent inhibitor of human adenovirus F41.

Author

Tollefson AE, Hussein ITM, Toth K, and Bowlin TL

Subjects

Humans, Child, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Valganciclovir, Ganciclovir therapeutic use, Cidofovir pharmacology, Adenoviruses, Human

Abstract

Clusters of acute non HepA-E hepatitis cases in previously healthy children have been reported globally. At least, 1010 cases were identified in 35 countries, 5% of those cases required liver transplantation and 2% died. The exact cause is not yet known, but there is circumstantial evidence suggesting that human adenovirus F41 (HAdV-F41) might be playing a role. No antiviral drug has been approved for treating human adenovirus infections. Furthermore, HAdV-F41 is notoriously difficult to grow in cell culture, which hindered studying the efficacy of an antiviral compound against this virus. Here, we show that filociclovir (FCV), a nucleoside analog, is a potent inhibitor of HAdV-F41 in cell culture using 2 approaches, namely immunostaining of infected cells and virus yield reduction assay. The activity of FCV was compared to 3 other known antivirals: cidofovir (CDV), ganciclovir (GCV) and valganciclovir (VGCV). Among the 4 compounds examined in this study, FCV was the most potent, with an EC 50 of 3.5 μM. These compounds can be ranked by potency as follows: FCV > CDV > GCV ≥ VGCV. In addition, FCV was 10-fold more potent than CDV in a virus yield reduction assay. This report provides timely and valuable methodologies to the research community for testing antivirals against HAdV-F41. Our findings also support the continued development of FCV for various therapeutic applications, including pediatric hepatitis, if a causal relationship is firmly established in the future., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published

2022

15. Heterogeneity and viral replication fitness of HSV-1 clinical isolates with mutations in the thymidine kinase and DNA polymerase.

Author

Schalkwijk HH, Gillemot S, Reynders M, Selleslag D, Andrei G, and Snoeck R

Subjects

Humans, Thymidine Kinase genetics, Thymidine Kinase pharmacology, Thymidine Kinase therapeutic use, Foscarnet pharmacology, Cidofovir pharmacology, Drug Resistance, Viral genetics, Acyclovir pharmacology, Acyclovir therapeutic use, DNA-Directed DNA Polymerase genetics, DNA-Directed DNA Polymerase pharmacology, Antiviral Agents therapeutic use, Mutation, Virus Replication, Herpesvirus 1, Human genetics, Herpes Simplex drug therapy

Abstract

Background: Prolonged antiviral therapy in immunocompromised individuals can result in the emergence of (multi)drug-resistant herpes simplex virus 1 (HSV-1) infections, forming a therapeutic challenge., Objectives: To evaluate spatial and temporal differences in drug resistance of HSV-1 samples from a HSCT recipient and to determine the effect of resistance mutations on viral replication fitness., Patients and Methods: Five HSV-1 isolates were recovered from a HSCT recipient who suffered from persistent HSV-1 lesions, consecutively treated with aciclovir, foscarnet, cidofovir and a combination of ganciclovir and cidofovir. Spatial and temporal differences in HSV-1 drug resistance were evaluated genotypically [Sanger sequencing and next-generation sequencing (NGS) of the viral thymidine kinase (TK) and DNA polymerase (DP)] and phenotypically (plaque reduction assay). Viral replication fitness was determined by dual infection competition assays., Results: Rapid evolution to aciclovir and foscarnet resistance was observed due to acquisition of TK (A189V and R222H) and DP (L778M and L802F) mutations. Virus isolates showed heterogeneous populations, spatial virus compartmentalization and minor viral variants in three out of five isolates (detectable by NGS but not by Sanger sequencing). Mutations in the TK and DP genes did not alter replication fitness without drug pressure. TK and/or DP mutants influenced replication fitness under antiviral pressure and showed increased fitness under pressure of the drug they showed resistance to., Conclusions: The use of NGS and dual infection competition assays revealed rapid evolution of HSV-1 drug resistance in a HSCT recipient with spatial and temporal compartmentalization of viral variants that had altered replication fitness under antiviral pressure., (© The Author(s) 2022. Published by Oxford University Press on behalf of British Society for Antimicrobial Chemotherapy. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2022

16. An acyclic phosphonate prodrug of HPMPC is effective against VZV in skin organ culture and mice.

Author

Lloyd MG, Liu D, Lyu J, Fan J, Overhulse JM, Kashemirov BA, Prichard MN, McKenna CE, and Moffat JF

Subjects

Acyclovir pharmacology, Animals, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Cidofovir pharmacology, Herpesvirus 3, Human, Humans, Mice, Organ Culture Techniques, Viral Regulatory and Accessory Proteins, Organophosphonates pharmacology, Prodrugs pharmacology

Abstract

Varicella zoster virus (VZV) causes chicken pox and shingles and is prevalent worldwide. Acyclovir and penciclovir (and its prodrugs) are first-line treatments for VZV infections, but they are not highly potent against VZV and resistance may arise in immunocompromised people on long-term therapy. HPMPC (cidofovir) is active against VZV, but cidofovir is not approved for treating VZV diseases, is nephrotoxic, and is not orally bioavailable. Here, we present the synthesis and evaluation of USC-373, a phosphonate prodrug of HPMPC with activity against VZV and other DNA viruses. In cultured fibroblasts, it was potent against VZV Ellen laboratory strain and was not overtly toxic, with EC 50 of 4 nM and CC 50 of 0.20 μM, producing a selectivity index of 50. In ARPE-19 cells, USC-373 was effective against VZV-ORF57-Luc wild type strain and the acyclovir-resistant isogenic strain. In human skin organ culture, USC-373 formulated in cocoa butter and applied topically prevented VZV-ORF57-Luc spread without toxicity. In NuSkin mice with human skin xenografts, one daily dose of 3 mg/kg was effective by the subcutaneous route, and one daily dose of 10 mg/kg was effective by the oral route. Remarkably, a 10 mg/kg oral dose given every other day was also effective. USC-373 was well tolerated and mice did not lose weight or show signs of distress. The prodrug modifications of USC-373 increase the potency and oral bioavailability compared to its parent nucleoside analog, HPMPC., (Copyright © 2022 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2022

17. Targeting ectromelia virus and TNF/NF-κB or STAT3 signaling for effective treatment of viral pneumonia.

Author

Pandey P, Al Rumaih Z, Kels MJT, Ng E, Kc R, Chaudhri G, and Karupiah G

Subjects

Animals, Antiviral Agents pharmacology, Cell Line, Chlorocebus aethiops, Cidofovir pharmacology, Cytokines metabolism, Drug Evaluation, Preclinical, Drug Therapy, Combination, Ectromelia virus drug effects, Female, Lung drug effects, Lung metabolism, Mice, Inbred C57BL, NF-kappa B metabolism, Pneumonia, Viral metabolism, STAT3 Transcription Factor metabolism, Signal Transduction drug effects, Tumor Necrosis Factor-alpha antagonists & inhibitors, Viral Load drug effects, Mice, Anti-Inflammatory Agents, Non-Steroidal administration & dosage, Antiviral Agents therapeutic use, Cidofovir therapeutic use, Etanercept administration & dosage, Pneumonia, Viral drug therapy

Abstract

Viral causes of pneumonia pose constant threats to global public health, but there are no specific treatments currently available for the condition. Antivirals are ineffective when administered late after the onset of symptoms. Pneumonia is caused by an exaggerated inflammatory cytokine response to infection, but tissue necrosis and damage caused by virus also contribute to lung pathology. We hypothesized that viral pneumonia can be treated effectively if both virus and inflammation are simultaneously targeted. Combined treatment with the antiviral drug cidofovir and etanercept, which targets tumor necrosis factor (TNF), down-regulated nuclear factor kappa B-signaling and effectively reduced morbidity and mortality during respiratory ectromelia virus (ECTV) infection in mice even when treatment was initiated after onset of clinical signs. Treatment with cidofovir alone reduced viral load, but animals died from severe lung pathology. Treatment with etanercept had no effect on viral load but diminished levels of inflammatory cytokines and chemokines including TNF, IL-6, IL-1β, IL-12p40, TGF-β, and CCL5 and dampened activation of the STAT3 cytokine-signaling pathway, which transduces signals from multiple cytokines implicated in lung pathology. Consequently, combined treatment with a STAT3 inhibitor and cidofovir was effective in improving clinical disease and lung pathology in ECTV-infected mice. Thus, the simultaneous targeting of virus and a specific inflammatory cytokine or cytokine-signaling pathway is effective in the treatment of pneumonia. This approach might be applicable to pneumonia caused by emerging and re-emerging viruses, like seasonal and pandemic influenza A virus strains and severe acute respiratory syndrome coronavirus 2., Competing Interests: The authors declare no competing interest.

Published

2022

18. Antiviral susceptibility of recombinant Herpes simplex virus 1 strains with specific polymerase amino acid changes.

Author

Rose R, Brunnemann AK, Baukmann S, Bühler S, Fickenscher H, Sauerbrei A, Zell R, and Krumbholz A

Subjects

Acyclovir pharmacology, Animals, Chlorocebus aethiops, Cidofovir pharmacology, Drug Resistance, Viral drug effects, Foscarnet pharmacology, Guanine pharmacology, Humans, Immunocompromised Host, Microbial Sensitivity Tests, Thymidine Kinase drug effects, Vero Cells, Antiviral Agents pharmacology, DNA-Directed DNA Polymerase drug effects, Herpes Simplex drug therapy, Herpesvirus 1, Human drug effects, Herpesvirus 1, Human genetics

Abstract

Acyclovir (ACV) and penciclovir and their prodrugs are recommended for therapy or prophylaxis of Herpes simplex virus 1 (HSV-1) infections. Their administration, however, can lead to the emergence of resistant strains with altered viral thymidine kinase (TK) function, especially in immunocompromised patients. Furthermore, amino acid (aa) changes of the viral deoxyribonucleic acid polymerase (POL) may contribute to resistance to the aforementioned nucleoside analogues. Given this, treatment with foscarnet (FOS) or cidofovir (CDV) may represent an important alternative. Both drugs directly affect POL activity. Several aa changes of POL, such as L49I, E70K, L359I, E421V, P829S, T1121M, and M1226I, have been observed in ACV-resistant clinical strains which also carried relevant aa changes in their TK. Their contribution to ACV, FOS, and CDV resistance is not fully understood. In this study, these seven aa changes with unknown significance for ACV, FOS and CDV resistance were introduced separately into the POL of a recombinant HSV-1 strain rHSV-1(17+)Lox, equipped with or without information for expression of green fluorescent protein (GFP). The GFP-expressing variants were tested for susceptibility to ACV, FOS and CDV. An rHSV-1(17+)Lox GFP strain with the S724N change conferring resistance to ACV and FOS was generated and included as a control. Only the S724N change was confirmed to induce ACV and FOS resistance, whereas the other changes did not contribute to resistance. The underlying nucleotide substitutions of the POL gene should be therefore considered as natural polymorphism. These data will improve sequence-based prediction of antiviral susceptibility., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

19. Assessment of Cidofovir for Treatment of Ocular Bovine Herpesvirus-1 Infection in Cattle Using an Ex-Vivo Model.

Author

Alling CR, Liu CC, Langohr IM, Haque M, Carter RT, Baker RE, and Lewin AC

Subjects

Administration, Ophthalmic veterinary, Animals, Antiviral Agents pharmacology, Cattle, Cattle Diseases virology, Cidofovir administration & dosage, Ganciclovir administration & dosage, Ganciclovir pharmacology, Herpesviridae Infections virology, Herpesvirus 1, Bovine pathogenicity, Herpesvirus 1, Bovine physiology, Cidofovir pharmacology, Herpesviridae Infections drug therapy, Herpesvirus 1, Bovine drug effects

Abstract

Bovine herpesvirus-1 (BoHV-1) infection contributes to keratoconjunctivitis, respiratory disease, and reproductive losses in cattle. The objective of this study was to determine the most appropriate ophthalmic antiviral agent for BoHV-1 inhibition using in-vitro culture and novel ex-vivo bovine corneal modeling. Half-maximal inhibitory concentrations of BoHV-1 were determined for cidofovir, ganciclovir, idoxuridine, and trifluridine via in-vitro plaque reduction assays. In-vitro cytotoxicity was compared amongst these compounds via luciferase assays. Trifluridine and cidofovir were the most potent BoHV-1 inhibitors in vitro, while trifluridine and idoxuridine were the most cytotoxic agents. Therefore, cidofovir was the most potent non-cytotoxic agent and was employed in the ex-vivo corneal assay. Corneoscleral rings ( n = 36) from fresh cadaver bovine globes were harvested and equally divided into an uninfected, untreated control group; a BoHV-1-infected, untreated group; and a BoHV-1-infected, cidofovir-treated group. Virus isolation for BoHV-1 titers was performed from corneal tissue and liquid media. Histologic measurements of corneal thickness, epithelial cell density, and tissue organization were compared between groups. Substantial BoHV-1 replication was observed in infected, untreated corneas, but BoHV-1 titer was significantly reduced in cidofovir-treated (1.69 ± 0.08 × 10 3 PFU/mL) versus untreated (8.25 ± 0.25 × 10 5 PFU/mL, p < 0.0001) tissues by day 2 of culture. No significant differences in histologic criteria were observed between groups. In conclusion, cidofovir warrants further investigation as treatment for BoHV-1 keratoconjunctivitis, with future studies needed to assess in-vivo tolerability and efficacy.

Published

2021

20. Topical Astodrimer Sodium, a Non-Toxic Polyanionic Dendrimer, Demonstrates Antiviral Activity in an Experimental Ocular Adenovirus Infection Model.

Author

Romanowski EG, Yates KA, Paull JRA, Heery GP, and Shanks RMQ

Subjects

A549 Cells, Adenoviruses, Human drug effects, Adenoviruses, Human physiology, Administration, Topical, Animals, Cidofovir pharmacology, Dendrimers pharmacology, Disease Models, Animal, Female, Humans, Polylysine pharmacology, Rabbits, Treatment Outcome, Viral Load drug effects, Adenoviridae Infections drug therapy, Cidofovir administration & dosage, Dendrimers administration & dosage, Eye Infections, Viral drug therapy, Polylysine administration & dosage

Abstract

There is no approved antiviral therapy for adenovirus (HAdV) ocular infections. Astodrimer sodium (SPL7013) is a polyanionic dendrimer with antiviral activity. The current study evaluated the ocular tolerability and anti-adenoviral efficacy of topical SPL7013 in rabbit ocular models. In a tolerability study, rabbits were treated with 3% SPL7013, vehicle, or 0.5% cidofovir. Their eyes were graded using the Draize scale. In antiviral efficacy studies, HAdV5 inoculated eyes were treated with 3% SPL7013, vehicle, or 0.5% cidofovir. Eyes were cultured for the virus on days 0, 1, 3, 4, 5, 7, 9, 11, and 14. Viral titers were determined. There were no differences in Draize scores between 3% SPL7013 and vehicle on any day. Cidofovir produced significantly higher Draize scores on day 12 than SPL7013 and vehicle. The 3% SPL7013 and 0.5% cidofovir significantly reduced daily viral titers and positive cultures per total compared with vehicle on several different days. The 3% SPL7013 and 0.5% cidofovir significantly reduced the duration of HAdV5 shedding compared to vehicle. The 3% SPL7013 demonstrated significantly more antiviral activity compared with vehicle in the Ad5/NZW rabbit ocular model. The 3% SPL7013 induced "minimal" to "practically non-irritating" Draize scores in the ocular tolerability study. Further development of astodrimer sodium as a topical antiviral therapy for adenoviral ocular infections is indicated.

Published

2021

21. Antiviral Drugs Against Herpesviruses.

Author

Piret J and Boivin G

Subjects

Cidofovir pharmacology, Cytomegalovirus, Humans, Simplexvirus, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Drug Resistance, Viral genetics

Abstract

The discovery of the nucleoside analogue, acyclovir, represented a milestone in the management of infections caused by herpes simplex virus and varicella-zoster virus. Ganciclovir, another nucleoside analogue, was then used for the management of systemic and organ-specific human cytomegalovirus diseases. The pyrophosphate analogue, foscarnet, and the nucleotide analogue, cidofovir, have been approved subsequently and constitute the second-line antiviral drugs. However, the viral DNA polymerase is the ultimate target of all these antiviral agents with a possible emergence of cross-resistance between these drugs. Recently, letermovir that targets the viral terminase complex was approved for the prophylaxis of human cytomegalovirus infections in hematopoietic stem cell transplant recipients. Other viral targets such as the protein kinase and the helicase-primase complex are also evaluated for the development of novel potent inhibitors against herpesviruses., (© 2021. The Author(s), under exclusive license to Springer Nature Singapore Pte Ltd.)

Published

2021

22. Diphenyl diselenide and cidofovir present anti-viral activity against Bovine Alphaherpesvirus 2 in vitro and in a sheep model.

Author

Amaral BP, Cargnelutti JF, Mortari APG, Merchioratto I, Feio LM, Nogueira CW, Weiblen R, and Flores E

Subjects

Animals, Antiviral Agents therapeutic use, Benzene Derivatives therapeutic use, Cidofovir therapeutic use, Female, Herpes Simplex drug therapy, Mammary Glands, Animal immunology, Mammary Glands, Animal virology, Organoselenium Compounds therapeutic use, Sheep, Sheep Diseases virology, Virus Shedding drug effects, Antiviral Agents pharmacology, Benzene Derivatives pharmacology, Cidofovir pharmacology, Herpes Simplex veterinary, Herpesvirus 2, Bovine drug effects, Organoselenium Compounds pharmacology, Sheep Diseases drug therapy

Abstract

Bovine alphaherpesvirus 2 (BoHV-2) - the agent of bovine herpetic mamillitis (BHM) - is related to Human alphaherpesviruses 1 and 2 (HHV-1, HHV-2) and, as such, has been proposed as a model for vaccine and drug testing. We herein investigated the anti-viral activity in vitro against BoHV-2 of three anti-herpetic drugs: Cidofovir (CDV), Fanciclovir (FAM), Foscarnet (PFA), and diphenyl disselenide (Ph 2 Se 2 ) , a compound that has showed activity against HHV-2. Plaque reduction assays (PRA) revealed a significant reduction in viral plaques (p < 0.05) in cells treated with Ph 2 Se 2 (79.7% reduction) or CDV (62.8%). FAM treatment resulted in a slight decrease in plaque number (22.9%, p < 0.05); PFA showed no activity. The effects of Ph 2 Se 2 and CDV, alone or in combination, were investigated in ewes inoculated with BoHV-2 transdermally and submitted to daily topic treatment. Virus inoculated ewes developed lesions progressing through the stages of hyperemia, large papules or depressed dark areas, followed by scab formation. Treatment with Ph 2 Se 2 resulted in reduction in clinical score from day 10 pi onwards (P < 0.05), shortening of clinical course and reduction in duration of virus shedding (P < 0.05) compared to untreated controls. Combined treatment (Ph 2 Se 2  + CDV) and CDV alone, also led to clinical improvement (P < 0.05), yet less pronounced and delayed. These results are promising towards the use of Ph 2 Se 2 , alone or in combination with anti-herpetic drugs, in the treatment of udder and teat lesions produced by BoHV-2 in dairy cows., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2021

23. A library of nucleotide analogues terminate RNA synthesis catalyzed by polymerases of coronaviruses that cause SARS and COVID-19.

Author

Jockusch S, Tao C, Li X, Anderson TK, Chien M, Kumar S, Russo JJ, Kirchdoerfer RN, and Ju J

Subjects

Antiviral Agents chemistry, Antiviral Agents therapeutic use, Betacoronavirus enzymology, Betacoronavirus genetics, COVID-19, Cidofovir chemistry, Cidofovir pharmacology, Cidofovir therapeutic use, Coronavirus Infections drug therapy, Dideoxynucleosides chemistry, Dideoxynucleosides pharmacology, Dideoxynucleosides therapeutic use, Ganciclovir chemistry, Ganciclovir pharmacology, Ganciclovir therapeutic use, Guanine analogs & derivatives, Guanine chemistry, Guanine pharmacology, Guanine therapeutic use, Nucleotides chemistry, Nucleotides therapeutic use, Pandemics, Pneumonia, Viral drug therapy, Prodrugs chemistry, Prodrugs pharmacology, Prodrugs therapeutic use, RNA, Viral antagonists & inhibitors, RNA, Viral biosynthesis, Severe acute respiratory syndrome-related coronavirus genetics, SARS-CoV-2, Severe Acute Respiratory Syndrome drug therapy, Stavudine chemistry, Stavudine pharmacology, Stavudine therapeutic use, Valganciclovir chemistry, Valganciclovir pharmacology, Valganciclovir therapeutic use, Antiviral Agents pharmacology, Coronavirus Infections virology, Nucleotides pharmacology, Pneumonia, Viral virology, RNA-Dependent RNA Polymerase antagonists & inhibitors, Severe acute respiratory syndrome-related coronavirus enzymology, Severe Acute Respiratory Syndrome virology

Abstract

SARS-CoV-2, a member of the coronavirus family, is responsible for the current COVID-19 worldwide pandemic. We previously demonstrated that five nucleotide analogues inhibit the SARS-CoV-2 RNA-dependent RNA polymerase (RdRp), including the active triphosphate forms of Sofosbuvir, Alovudine, Zidovudine, Tenofovir alafenamide and Emtricitabine. We report here the evaluation of a library of nucleoside triphosphate analogues with a variety of structural and chemical features as inhibitors of the RdRps of SARS-CoV and SARS-CoV-2. These features include modifications on the sugar (2' or 3' modifications, carbocyclic, acyclic, or dideoxynucleotides) or on the base. The goal is to identify nucleotide analogues that not only terminate RNA synthesis catalyzed by these coronavirus RdRps, but also have the potential to resist the viruses' exonuclease activity. We examined these nucleotide analogues for their ability to be incorporated by the RdRps in the polymerase reaction and to prevent further incorporation. While all 11 molecules tested displayed incorporation, 6 exhibited immediate termination of the polymerase reaction (triphosphates of Carbovir, Ganciclovir, Stavudine and Entecavir; 3'-OMe-UTP and Biotin-16-dUTP), 2 showed delayed termination (Cidofovir diphosphate and 2'-OMe-UTP), and 3 did not terminate the polymerase reaction (2'-F-dUTP, 2'-NH 2 -dUTP and Desthiobiotin-16-UTP). The coronaviruses possess an exonuclease that apparently requires a 2'-OH at the 3'-terminus of the growing RNA strand for proofreading. In this study, all nucleoside triphosphate analogues evaluated form Watson-Crick-like base pairs. The nucleotide analogues demonstrating termination either lack a 2'-OH, have a blocked 2'-OH, or show delayed termination. Thus, these nucleotide analogues are of interest for further investigation to evaluate whether they can evade the viral exonuclease activity. Prodrugs of five of these nucleotide analogues (Cidofovir, Abacavir, Valganciclovir/Ganciclovir, Stavudine and Entecavir) are FDA-approved medications for treatment of other viral infections, and their safety profiles are well established. After demonstrating potency in inhibiting viral replication in cell culture, candidate molecules can be rapidly evaluated as potential therapies for COVID-19., Competing Interests: Declaration of competing interest The authors declare no competing interests., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2020

24. In vitro co-infection by cytomegalovirus improves the antiviral activity of ganciclovir against human adenovirus.

Author

Aguilar-Guisado M, Marrugal-Lorenzo JA, Berastegui-Cabrera J, Merino L, Pachón J, and Sánchez-Céspedes J

Subjects

A549 Cells, Adenovirus Infections, Human drug therapy, Adenovirus Infections, Human virology, Adenoviruses, Human genetics, Antiviral Agents pharmacology, Cell Line, Coinfection drug therapy, Coinfection virology, Cytomegalovirus genetics, DNA, Viral metabolism, Humans, Inhibitory Concentration 50, Phosphorylation, Phosphotransferases (Alcohol Group Acceptor) chemistry, Adenoviruses, Human drug effects, Cidofovir pharmacology, Cytomegalovirus drug effects, Ganciclovir pharmacology

Abstract

Human adenovirus (HAdV) infection has an important clinical impact in the immunosuppressed population and is associated with high morbidity and mortality rates. The lack of a specific, safe and effective antiviral treatment against HAdV makes necessary the search for new therapeutic options. The aim of this study was to evaluate the in vitro activity of ganciclovir (GCV) against HAdV in co-infection by human cytomegalovirus (HCMV) and HAdV in cellular cultures. Quantitative real-time polymerase chain reaction (qPCR) was used to measure HAdV and HCMV DNA replication efficiency in monocultures and in co-infection situations in the presence of both cidofovir (CDV) and GCV. The effects of GCV and CDV were also evaluated in a burst assay (used to measure the production of virus particles) for both viruses, alone and in combination. GCV decreased by 1-log the HAdV DNA replication efficiency in co-infection with HCMV compared with its activity in HAdV monoculture. The burst assay showed that the reductions in virus yield in the presence of GCV were higher for HCMV and co-infection than for HAdV in monoculture (145.2±35.5- vs. 116.4±27.3- vs. 23.0±10.0-fold, respectively, P<0.05). The improved anti-HAdV activity of GCV during co-infection may be because of the more efficient phosphorylation of GCV by the HCMV protein kinase, UL97. Patients treated with GCV as pre-emptive therapy for HCMV infection may be considered as low-risk for developing HAdV infections; however, further evaluations are required to confirm these results., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

25. Acyclovir, cidofovir, and amenamevir have additive antiviral effects on herpes simplex virus TYPE 1.

Author

Greeley ZW, Giannasca NJ, Porter MJ, and Margulies BJ

Subjects

Animals, Chlorocebus aethiops, Drug Resistance, Viral, Drug Synergism, Herpesvirus 1, Human physiology, Inhibitory Concentration 50, Vero Cells, Acyclovir pharmacology, Antiviral Agents pharmacology, Cidofovir pharmacology, Herpesvirus 1, Human drug effects, Oxadiazoles pharmacology, Virus Replication drug effects

Abstract

Herpes simplex virus-1 (HSV-1) affects a large portion of the global population and has been shown to cause more severe symptoms in immunocompromised patients. It is in immunocompromised populations that HSV-1 has shown to have higher rates of resistance to the most commonly used antiherpetics, such as acyclovir/valacyclovir/penciclovir/famciclovir. The development of drug resistance has forced research into new antiherpetic therapies, including combination drug therapies. One potential complication of multidrug therapies is the existence of drug-drug interactions; as more drugs are used in the therapy, those interactions tend to become more complicated. This study tested the combination of acyclovir/cidofovir/amenamevir, the last drug being a new antiherpetic that targets the helicase-primase complex to prevent replication of viral DNA, for multidrug intervention. We used the design of experiments (DOE) function in Minitab to analyze the drug-drug interactions in their ability to inhibit growth of HSV-1. The DOE software was unable to detect any significant drug-drug interactions among these three antiherpetics as dosed. This would imply that these drugs could be used in combination to suppress viral replication without synergistic or antagonistic effects. This study shows that this therapy holds potential for further study and that DOE software is a potentially useful tool for determining complex drug-drug interactions., Competing Interests: Declaration of competing interest The authors declare no conflict of interest in this work., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2020

26. Effective Prophylactic Therapy for Exposure to Monkey B Virus ( Macacine alphaherpesvirus 1).

Author

Maxwell LK, Black DH, Wright GE, Breshears MA, and Eberle R

Subjects

Animals, Disease Models, Animal, Female, Humans, Mice, Inbred BALB C, Pre-Exposure Prophylaxis, Skin Diseases, Viral pathology, Skin Diseases, Viral prevention & control, Antiviral Agents pharmacology, Cidofovir pharmacology, Ganciclovir pharmacology, Herpesviridae Infections prevention & control, Herpesvirus 1, Cercopithecine drug effects, Mice

Abstract

Zoonotic monkey B virus ( Macacine alphaherpesvirus 1; BV) infections are extremely serious and usually fatal. Drugs currently used for treatment were developed for the treatment of herpes simplex virus but are less effective against BV. Effective suppression of viral replication in the skin could prevent the virus from invading the nervous system. To test this hypothesis, the efficacy of topical administration of several drugs against lethal BV infection was evaluated in female BALB/c mice that were infected by scarification. Drugs were then applied to the site of inoculation. As 3% preparations, most drugs were only minimally effective or ineffective. In contrast, ganciclovir and cidofovir were very effective. The ED 50 for cidofovir was 0.007%, compared with 1.1% for ganciclovir. At 0.5%, cidofovir protected against both death and neurologic signs, whereas 5% ganciclovir only protected against death but not neurologic involvement. All genotypes of BV were equally susceptible to cidofovir and ganciclovir. For maximal effectiveness, treatment with both cidofovir and ganciclovir had to be initiated within 8 h of infection. Cidofovir was completely protective when administered only on the day of infection, whereas a minimum of 5 d of treatment was required for maximal ganciclovir efficacy. These studies showed that topical cidofovir treatment started soon after BV exposure was very effective in preventing BV from invading the nervous system, whereas ganciclovir treatment was only partially effective. In addition, cidofovir was protective against a ganciclovir-resistant BV mutant, whereas ganciclovir was not. These studies showed that topical cidofovir treatment started soon after BV exposure is more effective than ganciclovir in preventing BV from invading the CNS.

Published

2020

27. Application of human lymphoid cells for the evaluation of antivirals against human adenovirus type 19: Zalcitabine has superior activity compared to cidofovir.

Author

Nakagawara K, Hayashi H, Kawaji K, Sasano M, and Kodama EN

Subjects

Adenoviruses, Human genetics, Cells, Cultured, Humans, Keratoconjunctivitis drug therapy, Keratoconjunctivitis virology, Lymphocytes virology, Microbial Sensitivity Tests, Adenoviruses, Human drug effects, Antiviral Agents pharmacology, Cidofovir pharmacology, Lymphocytes drug effects, Zalcitabine pharmacology

Abstract

Human adenovirus type 19 (HAdV-19) is a major cause of the epidemic keratoconjunctivitis. Outbreaks of keratoconjunctivitis are problematic to human health, especially for infants, the elderly, and immunocompromised individuals. However, the development of anti-HAdV drugs has been hampered by inconvenient screening systems; therefore, development of a simple screening method is highly desirable. In this study, we identified that HAdV-19 can infect a human lymphoid cell line transformed with human T-cell leukemia virus (MT-2 cells). MT-2 cells supported HAdV-19 replication and showed apparent cytopathic effects within five days post-infection. Using a thiazolyl blue tetrazolium bromide (MTT)-based colorimetric assay on MT-2 cells, we were able to detect the anti-HAdV-19 activities of previously reported nucleoside/tide compounds, including (S)-1-(3-hydroxy-2-phosphonylmethoxypropyl)cytosine (cidofovir), 2',3'-dideoxycytidine (zalcitabine) and 3'-deoxy-3'-fluorothymidine (trifluridine). Compared with previous methods, this system represents a more simple and rapid method to screen anti-HAdV-19 agents.

Published

2020

28. Artemisone demonstrates synergistic antiviral activity in combination with approved and experimental drugs active against human cytomegalovirus.

Author

Oiknine-Djian E, Bar-On S, Laskov I, Lantsberg D, Haynes RK, Panet A, and Wolf DG

Subjects

Acetates pharmacology, Benzimidazoles pharmacology, Cidofovir pharmacology, Cytosine analogs & derivatives, Cytosine pharmacology, Drug Interactions, Drug Synergism, Drugs, Investigational pharmacology, Female, Ganciclovir pharmacology, Humans, Organ Culture Techniques, Organophosphonates pharmacology, Placenta virology, Pregnancy, Quinazolines pharmacology, Ribonucleosides pharmacology, Antiviral Agents pharmacology, Artemisinins pharmacology, Cytomegalovirus drug effects, Cytomegalovirus Infections drug therapy

Abstract

We have recently shown that the artemisinin derivative artemisone, which was screened against malaria in human clinical studies, is a potent inhibitor of human cytomegalovirus (HCMV). Here we evaluated the antiviral effect of artemisone when employed in 2-drug combinations with approved and experimental anti-HCMV agents. Using the Chou-Talalay method, we found that in-vitro combination of artemisone with cidofovir, brincidofovir, or with the HCMV UL97 inhibitor maribavir resulted in antiviral synergism and the combination of artemisone with ganciclovir or with the viral terminase inhibitors letermovir and BDCRB resulted in moderate synergism. Importantly, the combination of artemisone with maribavir demonstrated synergistic antiviral activity ex-vivo, in a clinically-relevant multicellular model of human placental tissues maintained in organ culture. Our findings provide the basis for the use of artemisone in synergistically acting drug combinations, to enhance viral control and reduce antiviral drug toxicities., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

29. New 2-Oxoimidazolidine Derivatives: Design, Synthesis and Evaluation of Anti-BK Virus Activities in Vitro.

Author

Kornii Y, Chumachenko S, Shablykin O, Prichard MN, James SH, Hartline C, Zhirnov V, and Brovarets V

Subjects

Antiviral Agents chemical synthesis, Antiviral Agents chemistry, Cell Survival drug effects, Cells, Cultured, Cidofovir chemistry, Dose-Response Relationship, Drug, Humans, Imidazolidines chemical synthesis, Imidazolidines chemistry, Microbial Sensitivity Tests, Structure-Activity Relationship, Virus Replication drug effects, Antiviral Agents pharmacology, BK Virus drug effects, Cidofovir pharmacology, Drug Design, Imidazolidines pharmacology

Abstract

A series of novel 2-oxoimidazolidine derivatives were synthesized and their antiviral activities against BK human polyomavirus type 1 (BKPyV) were evaluated in vitro. Bioassays showed that the synthesized compounds 1-{[(4E)-5-(dichloromethylidene)-2-oxoimidazolidin-4-ylidene]sulfamoyl}piperidine-4-carboxylic acid (5) and N-Cyclobutyl-N'-[(4E)-5-(dichloromethylidene)-2-oxoimidazolidin-4-ylidene]sulfuric diamide (4) exhibited moderate activities against BKPyV (EC 50 =5.4 and 5.5 μm, respectively) that are comparable to the standard drug Cidofovir. Compound 5 exhibited the same cytotoxicity in HFF cells and selectivity index (SI 50 ) as Cidofovir. The selectivity index of compound 4 is three times less than that of Cidofovir due to the higher toxicity of this compound. Hence, these compounds may be taken as lead compound for further development of novel ant-BKPyV agents., (© 2019 Wiley-VHCA AG, Zurich, Switzerland.)

Published

2019

30. Cidofovir Diphosphate Inhibits Adenovirus 5 DNA Polymerase via both Nonobligate Chain Termination and Direct Inhibition, and Polymerase Mutations Confer Cidofovir Resistance on Intact Virus.

Author

Chamberlain JM, Sortino K, Sethna P, Bae A, Lanier R, Bambara RA, and Dewhurst S

Subjects

Adenovirus Infections, Human virology, Adenoviruses, Human enzymology, Adenoviruses, Human genetics, Adenoviruses, Human isolation & purification, Cytosine metabolism, Cytosine pharmacology, DNA Primers chemical synthesis, DNA Primers genetics, DNA, Viral biosynthesis, DNA, Viral genetics, DNA-Directed DNA Polymerase metabolism, Dose-Response Relationship, Drug, Humans, Kinetics, Mutation, Organophosphonates metabolism, Real-Time Polymerase Chain Reaction, Recombinant Proteins genetics, Recombinant Proteins metabolism, Viral Proteins metabolism, Virus Replication drug effects, Virus Replication genetics, Adenoviruses, Human drug effects, Antiviral Agents pharmacology, Cidofovir pharmacology, Cytosine analogs & derivatives, DNA, Viral antagonists & inhibitors, DNA-Directed DNA Polymerase genetics, Organophosphonates pharmacology, Viral Proteins genetics

Abstract

Human adenovirus (AdV) can cause fatal disease in immune-suppressed individuals, but treatment options are limited, in part because the antiviral cytidine analog cidofovir (CDV) is nephrotoxic. The investigational agent brincidofovir (BCV) is orally bioavailable, nonnephrotoxic, and generates the same active metabolite, cidofovir diphosphate (CDVpp). However, its mechanism of action against AdV is poorly understood. Therefore, we have examined the effect of CDVpp on DNA synthesis by a purified adenovirus 5 (AdV5) DNA polymerase (Pol). CDVpp was incorporated into nascent DNA strands and promoted a nonobligate form of chain termination (i.e., AdV5 Pol can extend, albeit inefficiently, a DNA chain even after the incorporation of a first CDVpp molecule). Moreover, unlike a conventional mismatched base pair, misincorporated CDVpp was not readily excised by the AdV5 Pol. At elevated concentrations, CDVpp inhibited AdV5 Pol in a manner consistent with both chain termination and direct inhibition of Pol activity. Finally, a recombinant AdV5 was constructed, containing Pol mutations (V303I and T87I) that were selected following an extended passage of wild-type AdV5 in the presence of BCV. This virus had a 2.1-fold elevated 50% effective concentration (EC 50 ) for BCV and a 1.9-fold increased EC 50 for CDV; thus, these results confirmed that viral resistance to BCV and CDV can be attributed to mutations in the viral Pol. These findings show that the anti-AdV5 activity of CDV and BCV is mediated through the viral DNA Pol and that their antiviral activity may occur via both (nonobligate) chain termination and (at high concentration) direct inhibition of AdV5 Pol activity., (Copyright © 2018 American Society for Microbiology.)

Published

2018

31. In vitro evaluation of current and novel antivirals in combination against human cytomegalovirus.

Author

O'Brien MS, Markovich KC, Selleseth D, DeVita AV, Sethna P, and Gentry BG

Subjects

Benzimidazoles pharmacology, Cell Line, Cidofovir pharmacology, Cyclopropanes pharmacology, Cytosine analogs & derivatives, Cytosine pharmacology, DNA-Directed DNA Polymerase drug effects, Drug Antagonism, Drug Combinations, Drug Resistance, Viral drug effects, Drug Resistance, Viral genetics, Drug Synergism, Drug Therapy, Combination, Endodeoxyribonucleases antagonists & inhibitors, Fibroblasts, Foscarnet pharmacology, Ganciclovir pharmacology, Guanine analogs & derivatives, Guanine pharmacology, Humans, Nucleic Acid Synthesis Inhibitors pharmacology, Organophosphonates pharmacology, Ribonucleosides pharmacology, Viral Proteins antagonists & inhibitors, Virus Replication drug effects, Antiviral Agents administration & dosage, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Cytomegalovirus drug effects, Cytomegalovirus Infections drug therapy

Abstract

Human cytomegalovirus (HCMV) can cause severe disease in patients with compromised or immature immune systems. Currently approved pharmacotherapies for the treatment of systemic HCMV infections [ganciclovir (GCV), cidofovir (CDV), foscarnet] are limited by a high incidence of adverse effects and/or the development of drug resistance. Given that many of these drugs have the same viral target (HCMV-encoded DNA polymerase), cross-resistance is relatively common. The primary means to combat drug resistance is combination pharmacotherapy using therapeutics with different molecular mechanisms of action with the expectation that those combinations result in an additive or synergistic enhancement of effect; combinations that result in antagonism can, in many cases, be detrimental to the outcome of the patient. We therefore tested select combinations of approved (GCV, CDV, letermovir (LMV)) and experimental (brincidofovir (BCV), cyclopropavir (CPV), maribavir (MBV), BDCRB) drugs with the hypothesis that combinations of drugs with different and distinct molecular mechanisms of action will produce an additive and/or synergistic enhancement of antiviral effect against HCMV in vitro. Using MacSynergy II (a statistical package that measures enhancement or lessening of effect relative to zero/additive), select drug combination studies demonstrated combination indices ranging from 160 to 372 with 95% confidence intervals greater than zero indicating that these combinations elicit a synergistic enhancement of effect against HCMV in vitro. These data suggest that administration of a viral DNA polymerase inhibitor, MBV, and/or a viral terminase inhibitor in combination has the potential to address the resistance/cross-resistance problems associated with currently available therapeutics., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

32. In vitro comparison of acyclovir, ganciclovir and cidofovir against equid alphaherpesvirus 3 and evaluation of their efficacy against six field isolates.

Author

Vissani MA, Zabal O, Tordoya MS, Parreño V, Thiry E, and Barrandeguy M

Subjects

Animals, Cells, Cultured, Female, Herpesviridae Infections virology, Herpesvirus 3, Equid isolation & purification, Horses, Acyclovir pharmacology, Antiviral Agents pharmacology, Cidofovir pharmacology, Ganciclovir pharmacology, Herpesviridae Infections veterinary, Herpesvirus 3, Equid drug effects, Horse Diseases virology

Abstract

Equid alphaherpesvirus 3 (EHV3) is the etiological agent of equine coital exanthema (ECE), which is a venereal, highly contagious disease, characterized by the formation of papules, vesicles, pustules and ulcers on the external genitalia of mares and stallions. EHV3 remains in a latent state after a successful infection and there are latently infected animals in which the virus is reactivated and generally re-excreted subclinically. There are no available vaccines for this condition and prevention is based on the clinical examination of mares prior to mating, which allows to segregate those showing clinical signs. As this approach does not eliminate the risk of contagion in stallions from subclinically infected mares, there is a need for a specific EHV3 treatment. Nowadays, there exist various antiviral compounds of proven effectiveness for other alphaherpesviruses affecting humans and animals. The aim of the present study was to compare the efficacy of three antiviral compounds, acyclovir, ganciclovir and cidofovir against EHV3 in vitro, and to assess their efficacy against six EHV3 Argentinian field isolates. To determine the efficacy of these compounds in vitro, three parameters were analyzed: reduction of plaque number, reduction of plaque size and reduction of viral production. Additionally, the effectiveness of the three compounds at an optimum concentration previously determined in this study was investigated for the EHV3 field isolates. Based on our results, ganciclovir was the most potent antiviral compound to reduce EHV3 replication in vitro and may thus be a valuable candidate for treatment and prevention of ECE in mares and stallions., (Copyright © 2018 Asociación Argentina de Microbiología. Publicado por Elsevier España, S.L.U. All rights reserved.)

Published

2018

33. Model of population pharmacokinetics of cidofovir in immunocompromised children with cytomegalovirus and adenovirus infection.

Author

Neant N, Klifa R, Bouazza N, Moshous D, Neven B, Leruez-Ville M, Blanche S, Treluyer JM, Hirt D, and Frange P

Subjects

Antiviral Agents administration & dosage, Antiviral Agents adverse effects, Antiviral Agents pharmacology, Area Under Curve, Blood Chemical Analysis, Child, Child, Preschool, Cidofovir administration & dosage, Cidofovir adverse effects, Cidofovir pharmacology, Drug-Related Side Effects and Adverse Reactions epidemiology, Female, Humans, Infant, Male, Treatment Outcome, Viral Load, Adenovirus Infections, Human drug therapy, Antiviral Agents pharmacokinetics, Cidofovir pharmacokinetics, Cytomegalovirus Infections drug therapy, Immunocompromised Host, Models, Statistical

Abstract

Objectives: To describe cidofovir pharmacokinetics and assess the link between concentration and safety/efficacy in children., Patients and Methods: An observational study was conducted in 13 immunocompromised children receiving cidofovir for adenovirus and/or cytomegalovirus infection. A population pharmacokinetic model was built and AUC0-24 was derived for each patient. Virological success was defined as a decrease of the viraemia by ≥1 log10 copies/mL within 15 days of cidofovir initiation. The association between AUC0-24 and virological success was assessed using a Wilcoxon test. An AUC0-24 cut-off value was determined using a Fisher's exact test., Results: Overall, 86 blood samples were analysed. A two-compartment model with first-order absorption and elimination best described the cidofovir data. Virological success (VS) was reached in 6/8 children with adenovirus viraemia and in 1/4 children with cytomegalovirus viraemia. Patients with VS displayed a non-significant higher median AUC0-24 compared with patients with virological failure: 48.6 (range 8.9-72.6) versus 19.1 (6.9-22.7) mg·h/L. Adenovirus-viraemic patients with an AUC0-24 value below 19.1 mg·h/L had a higher probability of treatment failure (P = 0.03). Aviraemic children with stool and/or nasopharyngeal adenovirus carriage cleared the viral carriage within a month of cidofovir initiation. During treatment, 1/13 children developed a tubulopathy but none of them had an increase in creatininaemia., Conclusions: Cidofovir appears safe and reasonably well tolerated and seemed to have efficacy in a subset of patients with adenovirus/cytomegalovirus infection. Therapeutic drug monitoring may be useful in children receiving cidofovir and, in the case of adenovirus infection, targeting an AUC0-24 above 19.1 mg·h/L could be associated with higher probability of virological success.

Published

2018

34. Efficacy of Cidofovir in Treatment of BK Virus-Induced Hemorrhagic Cystitis in Allogeneic Hematopoietic Cell Transplant Recipients.

Author

Coomes EA, Wolfe Jacques A, Michelis FV, Kim DDH, Thyagu S, Viswabandya A, Lipton JH, Messner HA, and Deotare U

Subjects

Adult, Aged, Antiviral Agents pharmacology, Cidofovir pharmacology, Cystitis drug therapy, Female, Hematopoietic Stem Cell Transplantation methods, Hemorrhagic Disorders drug therapy, Humans, Male, Middle Aged, Transplantation Conditioning methods, Antiviral Agents therapeutic use, BK Virus pathogenicity, Cidofovir therapeutic use, Cystitis chemically induced, Hematopoietic Stem Cell Transplantation adverse effects, Hemorrhagic Disorders chemically induced, Transplantation Conditioning adverse effects

Abstract

BK virus-associated hemorrhagic cystitis (BK-HC) is a common complication after allogeneic hematopoietic stem cell transplantation (allo-HCT), with incidences up to 70%. Cidofovir is an antiviral agent with growing evidence as a therapeutic intervention. To assess the safety profile and efficacy of intravenous and intravesical cidofovir in allo-HCT patients with BK-HC, a retrospective study was undertaken of the allo-HCT cohort who received cidofovir for symptomatic BK-HC (hematuria with BK viruria or viremia) from January 2010 until March 2017 in a single transplant center in Ontario, Canada. The primary outcome measure was a reduction in BK-HC severity (graded from 1 to 4); secondary outcomes included overall survival, BK virus titers, and the onset of acute kidney injury. Twelve allo-HCT patients received cidofovir for BK-HC, with pretreatment clinical severity of 3 (50%) or 4 (50%). Cidofovir was administered via intravenous (33%), intravesical (58%), or both modalities (8%). After a median cumulative dose of 10 mg/kg (range, 1 to 37), mean BK-HC grade decreased significantly by 1.8 (3.5 precidofovir, 1.7 postcidofovir, P < .01). Sixty-six percent of patients had at least partial response to cidofovir, with similar response rates between intravenous (66%) and intravesical (62%) administration. Sixty-seven percent of patients died, and 33% of patients experienced renal toxicity, including 2 patients receiving intravesical therapy. In this retrospective series, there was a significant reduction in BK-HC severity after cidofovir administration; most patients achieved at least partial response after cidofovir administration. Even with intravesical instillation, acute kidney injury remains a potential complication of cidofovir. Although cidofovir may be an efficacious therapy for BK-HC, albeit with potential demonstrated toxicities, further prospective trials are needed., (Copyright © 2018 The American Society for Blood and Marrow Transplantation. Published by Elsevier Inc. All rights reserved.)

Published

2018

35. Antiviral effect of the nucleoside analogue cidofovir in the context of sexual transmission of a gammaherpesvirus in mice.

Author

Zeippen C, Javaux J, Snoeck R, Neyts J, and Gillet L

Subjects

Animals, Female, Male, Mice, Inbred BALB C, Nucleosides analogs & derivatives, Post-Exposure Prophylaxis, Rhadinovirus physiology, Virus Latency, Virus Replication, Virus Shedding, Antiviral Agents pharmacology, Cidofovir pharmacology, Herpesviridae Infections drug therapy, Herpesviridae Infections transmission, Rhadinovirus drug effects, Sexually Transmitted Diseases, Viral drug therapy

Abstract

Objectives: To investigate the efficacy of cidofovir to block gammaherpesvirus replication in the context of sexual transmission., Methods: A luciferase-expressing strain of murid herpesvirus 4 (MuHV-4) was used to monitor genital virus excretion from infected female BALB/c mice and sexual transmission to naive males. The efficiency of cidofovir to block genital excretion from infected females or replication and host colonization of naive males after sexual contact was tested by treating infected females (either once daily or at a single timepoint), naive males before exposure (either once daily or at a single timepoint) or males 24 h post-exposure., Results: We showed that daily treatment of infected females can reduce MuHV-4 genital shedding by 75%. Similarly, daily preventive treatment of naive males was sufficient to block viral replication and latency establishment in males. In contrast, a single administration of cidofovir to infected females at day 14 post-infection or to naive males 2 to 6 days before contact with MuHV-4-excreting females was not sufficient to significantly reduce viral shedding from females or infection of males, respectively. Interestingly, a single administration of cidofovir to males 24 h after contact with MuHV-4-infected females excreting the virus in the genital tract significantly reduced virus replication in males and seroconversion., Conclusions: Altogether, our results show that cidofovir can significantly reduce gammaherpesvirus replication, excretion and colonization of the naive partner in the context of sexual transmission. Such treatments could therefore be recommended in some specific conditions where gammaherpesvirus infections could be deleterious.

Published

2018

36. In vitro susceptibility to ST-246 and Cidofovir corroborates the phylogenetic separation of Brazilian Vaccinia virus into two clades.

Author

Pires MA, Rodrigues NFS, de Oliveira DB, de Assis FL, Costa GB, Kroon EG, and Mota BEF

Subjects

Brazil, Humans, Phylogeny, Vaccinia drug therapy, Vaccinia virus genetics, Vaccinia virus physiology, Antiviral Agents pharmacology, Benzamides pharmacology, Cidofovir pharmacology, Isoindoles pharmacology, Vaccinia virology, Vaccinia virus classification, Vaccinia virus drug effects

Abstract

The Orthopoxvirus (OPV) genus of the Poxviridae family contains several human pathogens, including Vaccinia virus (VACV), which have been implicating in outbreaks of a zoonotic disease called Bovine Vaccinia in Brazil. So far, no approved treatment exists for OPV infections, but ST-246 and Cidofovir (CDV) are now in clinical development. Therefore, the objective of this work was to evaluate the susceptibility of five strains of Brazilian VACV (Br-VACV) to ST-246 and Cidofovir. The susceptibility of these strains to both drugs was evaluated by plaque reduction assay, extracellular virus's quantification in the presence of ST-246 and one-step growth curve in cells treated with CDV. Besides that, the ORFs F13L and E9L were sequenced for searching of polymorphisms associated with drug resistance. The effective concentration of 50% (EC 50 ) from both drugs varies significantly for different strains (from 0.0054 to 0.051 μM for ST-246 and from 27.14 to 61.23 μM for CDV). ST-246 strongly inhibits the production of extracellular virus for all isolates in concentrations as low as 0.1 μM and it was observed a relevant decrease of progeny production for all Br-VACV after CDV treatment. Sequencing of the F13L and E9L ORFs showed that Br-VACV do not present the polymorphism(s) associated with resistance to ST-246 and CDV. Taken together, our results showed that ST-246 and CDV are effective against diverse, wild VACV strains and that the susceptibility of Br-VACV to these drugs mirrored the phylogenetic split of these isolates into two groups. Thus, both ST-246 and CDV are of great interest as compounds to treat individuals during Bovine Vaccinia outbreaks in Brazil., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

37. Intravesical cidofovir application in BK virus cystitis after allogeneic hematopoetic stem cell transplantation (HSCT) is safe and highly effective.

Author

Mayer K, Schumacher M, Eis-Hübinger AM, Pietzonka S, Drosten C, Brossart P, and Wolf D

Subjects

Adult, Aged, Antiviral Agents therapeutic use, Cidofovir pharmacology, Cystitis virology, Female, Hematopoietic Stem Cell Transplantation, Humans, Male, Middle Aged, Polyomavirus Infections drug therapy, Retrospective Studies, Transplantation, Homologous, Treatment Outcome, BK Virus drug effects, Cidofovir administration & dosage, Cystitis drug therapy

Published

2018