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54. Favipiravir Inhibits Zika Virus (ZIKV) Replication in HeLa Cells by Altering Viral Infectivity.

Author

Franco, Evelyn J., Hanrahan, Kaley C., and Brown, Ashley N.

Subjects
ZIKA virus, HELA cells, CELL lines, CELL survival, CELLULAR therapy, DRUG side effects
Abstract

This study aims to evaluate the antiviral potential of the nucleoside analogue favipiravir (FAV) against ZIKV, an arbovirus for which there are no approved antiviral therapies, in three human-derived cell lines. HeLa (cervical), SK-N-MC (neuronal), and HUH-7 (liver) cells were infected with ZIKV and exposed to different concentrations of FAV. Viral supernatant was sampled daily, and infectious viral burden was quantified by plaque assay. Changes in ZIKV infectivity were quantified by calculating specific infectivity. FAV-related toxicities were also assessed for each cell line in both infected and uninfected cells. Our results demonstrate that FAV activity was most pronounced in HeLa cells, as substantial declines in infectious titers and viral infectivity were observed in this cell type. The decline in infectious virus occurred in an exposure-dependent manner and was more pronounced as FAV exposure times increased. Additionally, toxicity studies showed that FAV was not toxic to any of the three cell lines and, surprisingly, caused substantial improvements in the viability of infected HeLa cells. Although SK-N-MC and HUH-7 cells were susceptible to FAV's anti-ZIKV activity, similar effects on viral infectivity and improvements in cell viability with therapy were not observed. These results indicate that FAV's ability to substantially alter viral infectivity is host cell specific and suggest that the robust antiviral effect observed in HeLa cells is mediated through drug-induced losses of viral infectivity. [ABSTRACT FROM AUTHOR]

Published
2023
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55. Cytomegalovirus viremia and advanced HIV disease: is there an argument for anti-CMV treatment?

Author

Skipper, Caleb P. and Schleiss, Mark R.

Abstract

The role of cytomegalovirus (CMV) infection as a co-factor in HIV disease has been a topic of considerable interest since the beginning of the HIV pandemic. CMV is believed to function both as a co-factor in the progression of HIV infection, and as a contributor to enhanced disease for other opportunistic infections. In this special article, we review several recent studies that have enhanced our understanding of the role that CMV infection plays in the natural history of other HIV-related opportunistic infections. We review the clinical evidence that demonstrates how CMV viremia has emerged as an independent risk factor for the progression of infections such as those caused by C. neoformans and M. tuberculosis. We outline the biological underpinnings of the various hypotheses by which CMV, as an immunomodulatory virus, may modify the natural history of HIV-related infections. Evidence suggests that active CMV replication, manifest as CMV viremia (DNAemia), may play a key role in driving progression of HIV-associated opportunistic infections. We propose that control of CMV replication, independent of the known benefit of HAART therapy on reducing CMV end-organ disease, could reduce the risk of disease and mortality attributable to opportunistic infections such as cryptococcosis and tuberculosis. This could be achieved by the targeted use of CMV antivirals. The advent of newer (and safer) orally bioavailable CMV antivirals has renewed interest in, and opportunities for, randomized controlled trials to evaluate CMV viremia as a modifiable risk factor in high-risk persons with HIV disease. [ABSTRACT FROM AUTHOR]

Published
2023
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57. Effects of antiviral therapy and drug withdrawal on postpartum hepatitis in pregnant women with chronic HBV infection.

Author

Li, Minghui, Sun, Fangfang, Bi, Xiaoyue, Lin, Yanjie, Yang, Liu, Jiang, Tingting, Deng, Wen, Lu, Yao, Zhang, Lu, Yi, Wei, and Xie, Yao

Abstract

Objective: To investigate the effect of antiviral therapy and drug withdrawal on the incidence of hepatitis B after delivery in pregnant women with chronic hepatitis B virus (CHB) infection who received tenofovir disoproxil fumarate (TDF) treatment. Methods: Eligible CHB pregnant women were enrolled, and received TDF at 32 weeks gestation. The drug was stopped immediately or at 6 weeks after delivery. The HBV biomarkers and clinical biochemical parameters were monitored during gestation and 24 weeks after delivery. Results: There were 264 women completed the observation, including 96 untreated subjects in control group. Among 168 treated subjects, 131 cases stopped drug immediately after delivery and 37 cases delayed the drug withdrawal at 6 weeks after delivery. The incidence of postpartum hepatitis in control, immediate drug withdrawal, and delayed drug withdrawal were 28.1% (27/96), 23.7% (31/131), and 24.3% (9/37), showing no significant difference (χ2 = 0.607, p = 0.738). No factor was found to be associated with the occurrence of postpartum hepatitis. It's noteworthy that 96.3% of postpartum hepatitis in control group and 92.3% of postpartum hepatitis in immediate drug withdrawal group occurred within 12 weeks after delivery. While in delayed drug withdrawal group, the rate of postpartum hepatitis occurred within 12 weeks after delivery was 77.7%. Conclusion: Withdrawing antiviral drug immediately or at 6 weeks after delivery did not affect the incidence of postpartum hepatitis in CHB women, but delaying drug withdrawal might delay the onset of postpartum hepatitis. Clinical trial registration number: NCT03214302. [ABSTRACT FROM AUTHOR]

Published
2023
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58. Anti‐SARS‐CoV‐2 activity of targeted kinase inhibitors: Repurposing clinically available drugs for COVID‐19 therapy.

Author

Boytz, RuthMabel, Słabicki, Mikołaj, Ramaswamy, Sita, Patten, J. J., Zou, Charles, Meng, Chengcheng, Hurst, Brett L., Wang, Jinhua, Nowak, Radosław P., Yang, Priscilla L., Sattler, Martin, Stone, Richard M., Griffin, James D., Gray, Nathanael S., Gummuluru, Suryaram, Davey, Robert A., and Weisberg, Ellen

Subjects
SARS-CoV-2, KINASE inhibitors, COVID-19 treatment, COVID-19, CORONAVIRUS diseases, DRUG therapy
Abstract

Coronavirus disease 2019 (COVID‐19) remains a major public health concern, and vaccine unavailability, hesitancy, or failure underscore the need for discovery of efficacious antiviral drug therapies. Numerous approved drugs target protein kinases associated with viral life cycle and symptoms of infection. Repurposing of kinase inhibitors is appealing as they have been vetted for safety and are more accessible for COVID‐19 treatment. However, an understanding of drug mechanism is needed to improve our understanding of the factors involved in pathogenesis. We tested the in vitro activity of three kinase inhibitors against severe acute respiratory syndrome coronavirus 2 (SARS‐CoV‐2), including inhibitors of AXL kinase, a host cell factor that contributes to successful SARS‐CoV‐2 infection. Using multiple cell‐based assays and approaches, gilteritinib, nintedanib, and imatinib were thoroughly evaluated for activity against SARS‐CoV‐2 variants. Each drug exhibited antiviral activity, but with stark differences in potency, suggesting differences in host dependency for kinase targets. Importantly, for gilteritinib, the amount of compound needed to achieve 90% infection inhibition, at least in part involving blockade of spike protein‐mediated viral entry and at concentrations not inducing phospholipidosis (PLD), approached a clinically achievable concentration. Knockout of AXL, a target of gilteritinib and nintedanib, impaired SARS‐CoV‐2 variant infectivity, supporting a role for AXL in SARS‐CoV‐2 infection and supporting further investigation of drug‐mediated AXL inhibition as a COVID‐19 treatment. This study supports further evaluation of AXL‐targeting kinase inhibitors as potential antiviral agents and treatments for COVID‐19. Additional mechanistic studies are needed to determine underlying differences in virus response. [ABSTRACT FROM AUTHOR]

Published
2023
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59. Clinical study of ganshuang granule combined with tenofovir in the treatment of chronic hepatitis B complicated with nonalcoholic fatty liver disease.

Author

Changtian Su and Qin Yang

Subjects
NON-alcoholic fatty liver disease, CHRONIC hepatitis B, FATTY liver, TENOFOVIR, BODY mass index
Abstract

Objective: This study aims to investigate the clinical efficacy of Ganshuang granules combined with tenofovir, an antiviral drug, in the treatment of chronic hepatitis B complicated with nonalcoholic fatty liver disease. Methods: A total of 92 patients with chronic hepatitis B combined with nonalcoholic fatty liver who were treated in our Hospital from January 2020 to December 2021 were included as the research objects. According to the method of random number table, the patients were divided into the control group (n = 42) and the treatment group (n = 50). The control group was treated with silibinin meglumine tablets and tenofovir, while the treatment group was treated with Ganshuang granules combined with silybin meglumine tablets and tenofovir. Before and after treatment, liver function index, liver hardness measurement (LSM), controlled attenuation parameter (CAP), HBV-DNA serum load and body mass index (BMI) were observed. Results: Compared with the baseline, ALT, AST and GGT were significantly improved in both groups after treatment (p < 0.05), while TBIL indexes were not significantly different before and after treatment (p > 0.05). Patients in the treatment group had significantly lower ALT and AST index values than the control group at 12 and 24 weeks of treatment (p < 0.05). At 12 and 24 weeks of treatment, the fat attenuation parameters of the two groups were significantly decreased compared with those before treatment, and the difference was statistically significant (p < 0.05). The fat attenuation parameters in the treatment group were significantly lower than those in the control group at 12 and 24 weeks after treatment (p < 0.05). Conclusion: The effect of Ganshuang granule combined with antiviral drugs in the treatment of chronic hepatitis B complicated with non-alcoholic fatty liver is significantly better than that of antiviral drugs alone, which is worthy of clinical recommendation. [ABSTRACT FROM AUTHOR]

Published
2022
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60. Triazavirin—A Novel Effective Antiviral Drug.

Author

Chupakhin, Oleg N., Rusinov, Vladimir L., Varaksin, Mikhail V., Ulomskiy, Evgeny N., Savateev, Konstantin V., Butorin, Ilya I., Du, Weijie, Sun, Zhiyong, and Charushin, Valery N.

Subjects
RIFT Valley fever, WEST Nile fever, ANTIVIRAL agents, COVID-19, TICK-borne encephalitis
Abstract

This review outlines the data of numerous studies relating to the broad-spectrum antiviral drug Triazavirin that was launched on the Russian pharmaceutical market in 2014 as an anti-influenza drug (the international non-patented name is Riamilovir). The range of antiviral activity of Triazavirin has been significantly expanded during recent years; in particular, it has been shown that Triazavirin exhibits activity against tick-borne encephalitis, Rift Valley fever, West Nile fever, and other infections of viral etiology. This drug has been approved for treatment of influenza and acute respiratory infections by the Russian Ministry of Health on the basis of comprehensive clinical trials involving over 450 patients. Triazavirin was found to be a highly effective and well-tolerated drug, allowing its over-the-counter sale. The recently published data on the use of Triazavirin in clinical practice for the treatment of patients with COVID-19 are discussed, with special attention paid to potential biological targets for this drug. [ABSTRACT FROM AUTHOR]

Published
2022
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61. A Robust Phenotypic High-Throughput Antiviral Assay for the Discovery of Rabies Virus Inhibitors

Author

Xinyu Wang, Winston Chiu, Hugo Klaassen, Arnaud Marchand, Patrick Chaltin, Johan Neyts, and Dirk Jochmans

Subjects
rabies virus, high-throughput screening, drug repurposing, antiviral therapy, Microbiology, QR1-502
Abstract

Rabies virus (RABV) causes severe neurological symptoms in mammals. The disease is almost inevitably lethal as soon as clinical symptoms appear. The use of rabies immunoglobulins (RIG) and vaccination in post-exposure prophylaxis (PEP) can provide efficient protection, but many people do not receive this treatment due to its high cost and/or limited availability. Highly potent small molecule antivirals are urgently needed to treat patients once symptoms develop. In this paper, we report on the development of a high-throughput phenotypic antiviral screening assay based on the infection of BHK-21 cells with a fluorescent reporter virus and high content imaging readout. The assay was used to screen a repurposing library of 3681 drugs (all had been studied in phase 1 clinical trials). From this series, salinomycin was found to selectively inhibit viral replication by blocking infection at the entry stage. This shows that a high-throughput assay enables the screening of large compound libraries for the purposes of identifying inhibitors of RABV replication. These can then be optimized through medicinal chemistry efforts and further developed into urgently needed drugs for the treatment of symptomatic rabies.

Published
2023
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62. The Battle for Survival: The Role of RNA Non-Canonical Tails in the Virus–Host Interaction

Author

Xianghui Wen, Ahsan Irshad, and Hua Jin

Subjects
mixed tail, uridylation, TENT4, TUT4/7, virus, antiviral therapy, Microbiology, QR1-502
Abstract

Terminal nucleotidyltransferases (TENTs) could generate a ‘mixed tail’ or ‘U-rich tail’ consisting of different nucleotides at the 3′ end of RNA by non-templated nucleotide addition to protect or degrade cellular messenger RNA. Recently, there has been increasing evidence that the decoration of virus RNA terminus with a mixed tail or U-rich tail is a critical way to affect viral RNA stability in virus-infected cells. This paper first briefly introduces the cellular function of the TENT family and non-canonical tails, then comprehensively reviews their roles in virus invasion and antiviral immunity, as well as the significance of the TENT family in antiviral therapy. This review will contribute to understanding the role and mechanism of non-canonical RNA tailing in survival competition between the virus and host.

Published
2023
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64. Application and Impact of Antiviral Therapy for Patients with HBV-Related Hepatocellular Carcinoma Receiving Sorafenib and Lenvatinib Treatment.

Author

Lee, I-Cheng, Lee, Pei-Chang, Chao, Yee, Chi, Chen-Ta, Wu, Chi-Jung, Hung, Yi-Ping, Su, Chien-Wei, Hou, Ming-Chih, and Huang, Yi-Hsiang

Subjects
HEPATOCELLULAR carcinoma, ANTIVIRAL agents, SORAFENIB, PROTEIN-tyrosine kinase inhibitors, OVERALL survival, PROGNOSIS, PEMETREXED
Abstract

Overall survival (OS) in patients with advanced hepatocellular carcinoma (HCC) has improved in the era of multi-line sequential therapy. The application of antiviral therapy and its impact on survival for patients with HBV-related HCC needs to be reassessed. The aim of this study was to evaluate the application and impact of antiviral therapy on survival for patients with HBV-related HCC receiving tyrosine kinase inhibitor (TKI) therapy. Patients with advanced HBV-related HCC treated with sorafenib or lenvatinib as first-line therapy with (n = 377) and without (n = 182) nucleos(t)ide analogue (NUC) therapy were retrospectively enrolled. Prognostic factors of OS were evaluated. Secular trends in the increased application of NUC therapy and improved survival were observed in the last decade. The HBV reactivation rate in patients without NUC therapy was 6.6%. By multivariate analysis, baseline low HBV viral load, achieving undetectable HBV DNA after TKI therapy, and ability to receive second-line therapy were found to be independent predictors of OS. In subgroup patients with NUC therapy, starting NUC before TKI was associated with a better OS. In conclusion, the application of antiviral therapy for patients with HBV-related HCC receiving TKI therapy has increased over time. Achieving complete virological suppression may contribute to a better OS in patients with advanced HBV-related HCC. [ABSTRACT FROM AUTHOR]

Published
2022
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65. Antiviral strategies: What can we learn from natural reservoirs?

Author

Pan, Wenbo, Li, Weiwei, Liu, Lijing, and Zhang, Huawei

Subjects
TOMATO spotted wilt virus disease, CUCUMBER mosaic virus, PLANT breeding, PLANT viruses, ANTIVIRAL agents, PLANT diseases
Abstract

SUMMARY: Viruses cause many severe diseases in both plants and animals, urging us to explore new antiviral strategies. In their natural reservoirs, viruses live and replicate while causing mild or no symptoms. Some animals, such as bats, are the predicted natural reservoir of multiple viruses, indicating that they possess broad‐spectrum antiviral capabilities. Mechanisms of host defenses against viruses are generally studied independently in plants and animals. In this article, we speculate that some antiviral strategies of natural reservoirs are conserved between kingdoms. To verify this hypothesis, we created null mutants of 10‐formyltetrahydrofolate synthetase (AtTHFS), an Arabidopsis thaliana homologue of methylenetetrahydrofolate dehydrogenase, cyclohydrolase and formyltetrahydrofolate synthetase 1 (MTHFD1), which encodes a positive regulator of viral replication in bats. We found that disruption of AtTHFS enhanced plant resistance to three different types of plant viruses, including the tomato spotted wilt virus (TSWV), the cucumber mosaic virus (CMV) and the beet severe curly top virus (BSCTV). These results demonstrate a novel antiviral strategy for plant breeding. We further discuss the approaches used to identify and study natural reservoirs of plant viruses, especially those hosting many viruses, and highlight the possibility of discovering new antiviral strategies from them for plant molecular breeding and antiviral therapy. [ABSTRACT FROM AUTHOR]

Published
2022
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66. Traditional Chinese Medicine nursing for patients with skin rash caused by pegylated interferon α-2a combined with ribavirin therapy of chronic viral hepatitis C (慢性丙型肝炎患者聚乙二醇干扰素α-2a联合利巴韦林抗病毒治疗所致皮疹的中医护理体会)

Author

LI Hongyan (李红艳), WANG Xiaojun (汪晓军), and ZHANG Lili (张莉莉)

Subjects
interferon, antiviral therapy, skin rash, traditional chinese medicine nursing, psychological nursing, 干扰素, 抗病毒治疗, 皮疹, 中医护理, 心理护理, Nursing, RT1-120
Abstract

This paper analyzed the clinical data of 5 patients with skin rash caused by pegylated interferon α-2a combined with ribavirin therapy of chronic viral hepatitis C. According to the clinical symptoms, patients were given internal administration of Chinese herbal medicine decoction combined with external wash of Chinese herbal medicine decoction. Comprehensive interventions including skin care, infection prevention, nutrition support and psychological nursing were carried out during the treatment. (本文回顾聚乙二醇干扰素α-2a联合利巴韦林抗病毒治疗慢性丙型肝炎过程中出现皮疹(斑丘疹型)的5例患者的临床资料, 总结相关护理措施。结合患者中医证候表现, 辨证给予中药汤剂内服联合中药汤剂外洗患处, 同时配合实施皮肤护理、预防感染、营养支持、心理护理等措施。)

Published
2022
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73. Silicon Oxycarbide Porous Particles and Film Coating as Strategies for Tenofovir Controlled Release in Vaginal Tablets for HIV Prevention.

Author

Martín-Illana, Araceli, Cazorla-Luna, Raúl, Notario-Pérez, Fernando, Ruiz-Caro, Roberto, Rubio, Juan, Tamayo, Aitana, and Veiga, María Dolores

Subjects
HIV prevention, POROUS silicon, PORE size distribution, HIV infection transmission, DRUG tablets, TENOFOVIR, PROGESTERONE
Abstract

Sustained release of antiretroviral drugs is currently the most encouraging strategy for the prevention of the sexual transmission of HIV. Vaginal tablets based on hydrophilic gelling polymers are an interesting dosage form for this purpose, since they can be developed to modify the release of the drug depending on the tablet swelling. Tenofovir is a drug with proven activity in the prevention of HIV-1 infection, and it is possible to have it loaded in the surface of γ-aminopropyl trimethoxy silane-functionalized oxycarbide particles. These particles can be incorporated into the tablets, thus providing a sustained release of the drug. Moreover, the presence of the particles modifies the microstructure of the gel formed, as observed in scanning electron microscopy and Hg porosimetry studies, resulting into a gel with a narrow pore size distribution between 10 and 100 µm. This implies a lower volume of fluid incorporated into the gel during swelling studies, and therefore improved mucoadhesion times in ex vivo test. The coating of the formulations with Eudragit® RS modifies the swelling behavior of the tablets, which not only is decreased in magnitude but also extended in time, and as consequence the drug release is also prolonged for up to 7 days. [ABSTRACT FROM AUTHOR]

Published
2022
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74. The ZCCHC14/TENT4 complex is required for hepatitis A virus RNA synthesis.

Author

You Li, Ichiro Misumi, Tomoyuki Shiota, Lu Sun, Lenarcic, Erik M., Hyejeong Kim, Takayoshi Shirasaki, Hertel-Wulff, Adriana, Tibbs, Taylor, Mitchell, Joseph E., McKnight, Kevin L., Cameron, Craig E., Moorman, Nathaniel J., McGivern, David R., Cullen, John M., Whitmire, Jason K., and Lemon, Stanley M.

Subjects
HEPATITIS viruses, RNA synthesis, VIRAL hepatitis, RNA viruses, HEPATITIS A virus, VACCINE manufacturing
Abstract

Despite excellent vaccines, resurgent outbreaks of hepatitis A have caused thousands of hospitalizations and hundreds of deaths within the United States in recent years. There is no effective antiviral therapy for hepatitis A, and many aspects of the hepatitis A virus (HAV) replication cycle remain to be elucidated. Replication requires the zinc finger protein ZCCHC14 and noncanonical TENT4 poly(A) polymerases with which it associates, but the underlying mechanism is unknown. Here, we show that ZCCHC14 and TENT4A/B are required for viral RNA synthesis following translation of the viral genome in infected cells. Cross-linking immunoprecipitation sequencing (CLIP-seq) experiments revealed that ZCCHC14 binds a small stem-loop in the HAV 5′ untranslated RNA possessing a Smaug recognition-like pentaloop to which it recruits TENT4. TENT4 polymerases lengthen and stabilize the 3′ poly(A) tails of some cellular and viral mRNAs, but the chemical inhibition of TENT4A/B with the dihydroquinolizinone RG7834 had no impact on the length of the HAV 3′ poly(A) tail, stability of HAV RNA, or cap-independent translation of the viral genome. By contrast, RG7834 inhibited the incorporation of 5-ethynyl uridine into nascent HAV RNA, indicating that TENT4A/B function in viral RNA synthesis. Consistent with potent in vitro antiviral activity against HAV (IC50 6.11 nM), orally administered RG7834 completely blocked HAV infection in Ifnar1−/− mice, and sharply reduced serum alanine aminotransferase activities, hepatocyte apoptosis, and intrahepatic inflammatory cell infiltrates in mice with acute hepatitis A. These results reveal requirements for ZCCHC14-TENT4A/B in hepatovirus RNA synthesis, and suggest that TENT4A/B inhibitors may be useful for preventing or treating hepatitis A in humans. [ABSTRACT FROM AUTHOR]

Published
2022
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75. New Targets for Antiviral Therapy: Inhibitory Receptors and Immune Checkpoints on Myeloid Cells.

Author

Liu, Yanni, Nicklin, Paul, and He, Yuan

Subjects
MYELOID cells, IMMUNE checkpoint proteins, CELL receptors, TRANSMISSIBLE tumors, CELLULAR control mechanisms, KILLER cells, HOMEOSTASIS
Abstract

Immune homeostasis is achieved by balancing the activating and inhibitory signal transduction pathways mediated via cell surface receptors. Activation allows the host to mount an immune response to endogenous and exogenous antigens; suppressive modulation via inhibitory signaling protects the host from excessive inflammatory damage. The checkpoint regulation of myeloid cells during immune homeostasis raised their profile as important cellular targets for treating allergy, cancer and infectious disease. This review focuses on the structure and signaling of inhibitory receptors on myeloid cells, with particular attention placed on how the interplay between viruses and these receptors regulates antiviral immunity. The status of targeting inhibitory receptors on myeloid cells as a new therapeutic approach for antiviral treatment will be analyzed. [ABSTRACT FROM AUTHOR]

Published
2022
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79. Non-nucleoside structured compounds with antiviral activity—past 10 years (2010–2020).

Author

Denel-Bobrowska, Marta and Olejniczak, Agnieszka B.

Subjects
*ANTIVIRAL agents, *NUCLEOSIDE derivatives, *ANTIVIRAL nucleosides, *DRUG target, *DRUG repositioning, *DRUG development, *DRUG approval
Abstract

Nucleosides and their derivatives are a well-known and well-described class of compounds with antiviral activity. Currently, in the era of the COVID-19 pandemic, scientists are also looking for compounds not related to nucleosides with antiviral properties. This review aims to provide an overview of selected synthetic antiviral agents not associated to nucleosides developed against human viruses and introduced to preclinical and clinical trials as well as drugs approved for antiviral therapy over the last 10 years. The article describes for the first time the wide classification of such antiviral drugs and drug candidates and briefly summarizes the biological target and clinical applications of the compounds. The described compounds are arranged according to the antiviral mechanism of action. Knowledge of the drug's activity toward specific molecular targets may be the key to researching new antiviral compounds and repositioning drugs already approved for clinical use. The paper also briefly discusses the future directions of antiviral therapy. The described examples of antiviral compounds can be helpful for further drug development. [Display omitted] • Non-nucleoside structured compounds with antiviral activity. • Molecular mechanisms of action of antiviral agents. • Antiviral agents tested in preclinical or clinical trials. • Antiviral non-nucleoside structured drugs approved by FDA in 2010–2020. [ABSTRACT FROM AUTHOR]

Published
2022
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80. Treatment Options for Hepatitis A and E: A Non-Systematic Review

Author

Filippo Gabrielli, Francesco Alberti, Cristina Russo, Carmela Cursaro, Hajrie Seferi, Marzia Margotti, and Pietro Andreone

Subjects
hepatitis A virus, HAV, hepatitis E virus, HEV, treatment, antiviral therapy, Microbiology, QR1-502
Abstract

Hepatitis A and hepatitis E are relatively common causes of liver disease. Both viruses are mainly transmitted through the faecal–oral route and, consequently, most outbreaks occur in countries with poor sanitation. An important role of the immune response as the driver of liver injury is also shared by the two pathogens. For both the hepatitis A (HAV) and hepatitis E (HEV) viruses, the clinical manifestations of infection mainly consist of an acute disease with mild liver injury, which results in clinical and laboratory alterations that are self-limiting in most cases. However, severe acute disease or chronic, long-lasting manifestations may occur in vulnerable patients, such as pregnant women, immunocompromised individuals or those with pre-existing liver disease. Specifically, HAV infection rarely results in fulminant hepatitis, prolonged cholestasis, relapsing hepatitis and possibly autoimmune hepatitis triggered by the viral infection. Less common manifestations of HEV include extrahepatic disease, acute liver failure and chronic HEV infection with persistent viraemia. In this paper, we conduct a non-systematic review of the available literature to provide a comprehensive understanding of the state of the art. Treatment mainly consists of supportive measures, while the available evidence for aetiological treatment and additional agents in severe disease is limited in quantity and quality. However, several therapeutic approaches have been attempted: for HAV infection, corticosteroid therapy has shown outcome improvement, and molecules, such as AZD 1480, zinc chloride and heme oxygenase-1, have demonstrated a reduction in viral replication in vitro. As for HEV infection, therapeutic options mainly rely on the use of ribavirin, and some studies utilising pegylated interferon-alpha have shown conflicting results. While a vaccine for HAV is already available and has led to a significant reduction in the prevalence of the disease, several vaccines for HEV are currently being developed, with some already available in China, showing promising results.

Published
2023
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81. Spectrum of Atazanavir-Selected Protease Inhibitor-Resistance Mutations.

Author

Rhee, Soo-Yon, Boehm, Michael, Tarasova, Olga, Di Teodoro, Giulia, Abecasis, Ana B., Sönnerborg, Anders, Bailey, Alexander J., Kireev, Dmitry, Zazzi, Maurizio, and Shafer, Robert W.

Subjects
PROTEASE inhibitors, ATAZANAVIR, ANTI-HIV agents, MIDDLE-income countries, DRUG resistance, DARUNAVIR, HIV, MUPIROCIN
Abstract

Ritonavir-boosted atazanavir is an option for second-line therapy in low- and middle-income countries (LMICs). We analyzed publicly available HIV-1 protease sequences from previously PI-naïve patients with virological failure (VF) following treatment with atazanavir. Overall, 1497 patient sequences were identified, including 740 reported in 27 published studies and 757 from datasets assembled for this analysis. A total of 63% of patients received boosted atazanavir. A total of 38% had non-subtype B viruses. A total of 264 (18%) sequences had a PI drug-resistance mutation (DRM) defined as having a Stanford HIV Drug Resistance Database mutation penalty score. Among sequences with a DRM, nine major DRMs had a prevalence >5%: I50L (34%), M46I (33%), V82A (22%), L90M (19%), I54V (16%), N88S (10%), M46L (8%), V32I (6%), and I84V (6%). Common accessory DRMs were L33F (21%), Q58E (16%), K20T (14%), G73S (12%), L10F (10%), F53L (10%), K43T (9%), and L24I (6%). A novel nonpolymorphic mutation, L89T occurred in 8.4% of non-subtype B, but in only 0.4% of subtype B sequences. The 264 sequences included 3 (1.1%) interpreted as causing high-level, 14 (5.3%) as causing intermediate, and 27 (10.2%) as causing low-level darunavir resistance. Atazanavir selects for nine major and eight accessory DRMs, and one novel nonpolymorphic mutation occurring primarily in non-B sequences. Atazanavir-selected mutations confer low-levels of darunavir cross resistance. Clinical studies, however, are required to determine the optimal boosted PI to use for second-line and potentially later line therapy in LMICs. [ABSTRACT FROM AUTHOR]

Published
2022
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82. CRISPR/Cas13-assisted hepatitis B virus covalently closed circular DNA detection.

Author

Zhang, Xiangying, Tian, Yuan, Xu, Ling, Fan, Zihao, Cao, Yaling, Ma, Yingmin, Li, Hao, and Ren, Feng

Abstract

Background and aims: The formation of an intranuclear pool of covalently closed circular DNA (cccDNA) in the liver is the main cause of persistent hepatitis B virus (HBV) infection. Here, we established highly sensitive and specific methods to detect cccDNA based on CRISPR-Cas13a technology. Methods: We used plasmid-safe ATP-dependent DNase (PSAD) enzymes and HindIII to digest loose circle rcDNA and double-stranded linear DNA, amplify specific HBV cccDNA fragments by rolling circle amplification (RCA) and PCR, and detect the target gene using CRISPR-Cas13a technology. The CRISPR-Cas13a-based assay for the detection of cccDNA was further clinically validated using HBV-related liver tissues, plasma, whole blood and peripheral blood mononuclear cells (PBMCs). Results: Based on the sample pretreatment step, the amplification step and the detection step, we established a new CRISPR-Cas13a-based assay for the detection of cccDNA. After the amplification of RCA and PCR, 1 copy/μl HBV cccDNA could be detected by CRISPR/Cas13-assisted fluorescence readout. We used ddPCR, qPCR, RCA-qPCR, PCR-CRISPR and RCA-PCR-CRISPR methods to detect 20, 4, 18, 14 and 29 positive samples in liver tissue samples from 40 HBV-related patients, respectively. HBV cccDNA was almost completely undetected in the 20 blood samples of HBV patients (including plasma, whole blood and PBMCs) by the above 5 methods. Conclusions: We developed a novel CRISPR-based assay for the highly sensitive and specific detection of HBV cccDNA, presenting a promising alternative for accurate detection of HBV infection, antiviral therapy evaluation and treatment guidance. [ABSTRACT FROM AUTHOR]

Published
2022
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83. Cost-effectiveness of antiviral therapy in untreated compensated cirrhosis patient with serum HBV–DNA level < 2000 IU/mL.

Author

Lee, Hankil, Jang, Sungin, Ahn, Sang Hoon, and Kim, Beom Kyung

Abstract

Background: Due to stringent reimbursement criteria, significant numbers of patients with compensated cirrhosis (CC) and low-level viremia [LLV; serum hepatitis B virus (HBV)–DNA levels of 20–2000 IU/mL] remain untreated especially in the East Asian countries, despite potential risk of disease progression. We analyzed cost-effectiveness to assess rationales for antiviral therapy (AVT) for this population. Methods: We compared cost and effectiveness (quality-adjusted life years, QALYs) in a virtual cohort including 10,000 54-year-old CC-LLV patients receiving AVT (Scenario I) versus no treatment (Scenario II). A Markov model, including seven HBV-related conditions, was used. Values for transition probabilities and costs were mostly obtained from recent real-world South Korean data. Results: As per a simulation of a base-case analysis, AVT reduced costs by $639 USD and yielded 0.108 QALYs per patient for 5 years among CC-LLV patients compared to no treatment. Thus, AVT is a cost-saving option with lower costs and better effectiveness than no treatment. If 10,000 patients received AVT, 815 incident cases of hepatocellular carcinoma (HCC) and 630 HBV-related deaths could be averted in 5 years compared to no treatment. In case of 10-year observation, AVT was consistently dominant. Even when the transition probabilities from CC-LLV vs. maintained virological response to HCC were same, fluctuation of results also lied within willingness-to-pay in South Korea. In the probabilistic sensitivity analysis with the willingness-to-pay threshold, the probability of AVT cost-effectiveness was 100%. Conclusion: The extended application of AVT in CC-LLV patients may contribute positively to individual clinical benefits and national healthcare budgets. [ABSTRACT FROM AUTHOR]

Published
2022
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84. Long‐term renal safety between patients with chronic hepatitis B receiving tenofovir vs. entecavir therapy: A multicenter study.

Author

Chon, Young Eun, Park, Soo Young, Kim, Seung Up, Hong, Han Pyo, Lee, Jae Seung, Lee, Hye Won, Kim, Mi Na, Park, Jun Yong, Kim, Do Young, Ahn, Sang Hoon, and Kim, Beom Kyung

Subjects
CHRONIC hepatitis B, PATIENT safety, TENOFOVIR, CHRONIC kidney failure, GLOMERULAR filtration rate, EPIDERMAL growth factor receptors
Abstract

Renal safety is a critical issue in chronic hepatitis B (CHB) patients receiving long‐term entecavir (ETV) or tenofovir disofuroxil fumarate (TDF) therapy. We investigated their effects on estimated glomerular filtration rate (eGFR). Treatment‐naive CHB patients receiving ETV or TDF for ≥1 year were recruited. The eGFR was assessed using the Chronic Kidney Disease Epidemiology Collaboration equation. We calculated average annual percent change (AAPC) in eGFR using Joinpoint regression. At the beginning of the observation, the ETV group had more unfavorable conditions than the TDF group: lower eGFR and higher FIB‐4 and APRI than the TDF group (all p <.001). After 6 years of antiviral therapy, the mean eGFR in the ETV group (n = 1793) was maintained (96.0 at first year to 95.6 ml/min/1.73 m2 at sixth year; AAPC −0.09%; p =.322), whereas that in the TDF group (n = 1240) significantly decreased annually (101.9 at first year to 96.9 ml/min/1.73 m2 at sixth year; AAPC −0.88%; p <.001). Notably, in the TDF group, even patients without diabetes (AAPC −0.80%; p = 0.001) or hypertension (AAPC −0.87%; p =.001) experienced significant decrease in eGFR. Expectably, accompanying diabetes (AAPC −1.59%; p =.011) or hypertension (AAPC −1.00%; p =.002) tended to accelerate eGFR decrease. TDF treatment (odds ratio 1.66, p <.001), along with eGFR<60 ml/min/1.73 m2, serum albumin<3.5 mg/dl, and hypertension, were independently associated with ongoing renal dysfunction, defined as a negative slope of the mean eGFR change. In conclusion, compared with ETV, long‐term TDF treatment induced slow, but progressive renal dysfunction. Although the annual eGFR change by TDF was small, careful monitoring is necessary, especially in patients requiring life‐long therapy. [ABSTRACT FROM AUTHOR]

Published
2022
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85. Nanophysics in modern medicine.

Author

Lozovski, V. Z., Lysenko, V. S., and Rusinchuk, N. M.

Subjects
TARGETED drug delivery, ANTIVIRAL agents, PONDEROMOTIVE force, NANOSTRUCTURED materials, VIRAL envelopes, PHENOMENOLOGICAL theory (Physics), POLYMERSOMES
Abstract

Nanophysics is rapidly developing for the recent couple of decades. Unique physical properties of materials at the nanoscale are the reason for this rapid development. Ideas, materials and structures of nanophysics have found their wide application in related fields of modern science, including biology and medicine. This short review is devoted to the application of nanophysics in modern medicine. The main focus was on application of ideas and physical phenomena of nanophysics in oncology and antiviral therapy. We have focused on the use of nanosystems both for tumor imaging and for the struggle against some types of tumors. The use of nanoparticles as nanocontainers for targeted drug delivery was briefly discussed. We also demonstrated how the effects of nanophysics can be used to develop new non-traditional methods of antiviral therapy. The focus of these methods was the idea of physical (field) action of nanoparticles on the viruses, which is based on the local-field enhancement effect that is the reason of ponderomotive forces acting on the viruses up to destruction of viral envelopes. [ABSTRACT FROM AUTHOR]

Published
2022
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86. Characteristics and outcomes of patients with COVID-19 and liver injury: a retrospective analysis and a multicenter experience.

Author

Voiosu, Andrei, Roman, Adina, Pop, Ruxandra, Boeriu, Alina, Popp, Cristiana, Zurac, Sabina, Voiosu, Theodor, Dobru, Daniela, and Mateescu, Bogdan

Subjects
COVID-19, LIVER injuries, LIVER function tests, HEPATITIS, HYDROXYCHLOROQUINE
Abstract

Background and aims. Patients with COVID-19 frequently present abnormal elevated liver function tests of unknown clinical significance. We aimed to investigate the characteristics and factors influencing outcome in patients with confirmed SARS-CoV-2 infection and liver injury on admission. Methods. This is a retrospective observational study of patients hospitalized in two COVID units in Romania. Relevant data on clinical and laboratory parameters and medication administered during the admission were analyzed to identify predictors of a negative outcome. Patients with confirmed COVID-19 and liver function tests (LFTs) above the upper limit of normal were included in the analysis. Results. From 1,207 patients, we identified 134 patients (11%) with abnormal LFTs during hospitalization. The majority of patients had mildly elevated levels and a predominantly cholestatic pattern of liver injury. Patients who received lopinavir/ritonavir were more likely to have increased ALAT levels (p<0.0001). Sixteen patients had pre-existing chronic liver disease, and they were more likely to suffer from severe COVID-19 (p=0.009) and have a negative outcome (p<0.001), but on multivariate analysis, only the severity of COVID-19 was predictive of death (OR 69.9; 95% CI 6.4-761.4). Conclusions. Mild liver injury is relatively common in COVID-19 and possibly influenced by medication. Patients with chronic liver disease are at high risk for negative outcome, but the severity of the infection is the only predictor of death. [ABSTRACT FROM AUTHOR]

Published
2022
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87. Multiscale Model of Antiviral Timing, Potency, and Heterogeneity Effects on an Epithelial Tissue Patch Infected by SARS-CoV-2.

Author

Ferrari Gianlupi, Juliano, Mapder, Tarunendu, Sego, T. J., Sluka, James P., Quinney, Sara K., Craig, Morgan, Stratford Jr., Robert E., and Glazier, James A.

Subjects
EPITHELIUM, MULTISCALE modeling, SARS-CoV-2, COVID-19 treatment, VIRUS diseases, LUNGS
Abstract

We extend our established agent-based multiscale computational model of infection of lung tissue by SARS-CoV-2 to include pharmacokinetic and pharmacodynamic models of remdesivir. We model remdesivir treatment for COVID-19; however, our methods are general to other viral infections and antiviral therapies. We investigate the effects of drug potency, drug dosing frequency, treatment initiation delay, antiviral half-life, and variability in cellular uptake and metabolism of remdesivir and its active metabolite on treatment outcomes in a simulated patch of infected epithelial tissue. Non-spatial deterministic population models which treat all cells of a given class as identical can clarify how treatment dosage and timing influence treatment efficacy. However, they do not reveal how cell-to-cell variability affects treatment outcomes. Our simulations suggest that for a given treatment regime, including cell-to-cell variation in drug uptake, permeability and metabolism increase the likelihood of uncontrolled infection as the cells with the lowest internal levels of antiviral act as super-spreaders within the tissue. The model predicts substantial variability in infection outcomes between similar tissue patches for different treatment options. In models with cellular metabolic variability, antiviral doses have to be increased significantly (>50% depending on simulation parameters) to achieve the same treatment results as with the homogeneous cellular metabolism. [ABSTRACT FROM AUTHOR]

Published
2022
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89. Diagnosis, prevention, and treatment of coronavirus disease: a review.

Author

Sarangi, Manoj Kumar, Padhi, Sasmita, Dheeman, Shrivardhan, Karn, Santosh Kumar, Patel, L. D., Yi, Dong Kee, and Nanda, Sitansu Sekhar

Abstract

Coronavirus disease (COVID-19) was first reported in Wuhan, China, in late December 2019 and subsequently, declared a pandemic. As of 3 June 2021, 172,493,290 individuals have acquired COVID-19 and 3,708,334 patients have died worldwide, according to the World Health Organization. This review explores epidemiology; virology; pathogenesis; genomic variations; mode of transmission; clinical occurrence; diagnosis; and treatment with antiviral agents, antibiotics, and supportive therapies. It covers a nanotechnology-based treatment approach and emphasizes the importance of herbal and marine antiviral drugs. The review attempts to explain current advances in research, prevention, and control of COVID-19 spread through artificial intelligence and vaccine development status under cosmopolitan consideration. While COVID-19 research is advancing at full capacity, the discovery of drugs or vaccines that can fight the pandemic is necessary. Human survival in such a critical situation will be possible only with the development of strong immunity by opting for exercise, yoga, and consumption of hygienic food and beverages. Therefore, education about COVID-19 lethality and its impact on livelihood is important. The pandemic has also shown positive effects on the environment, such as a significant reduction in environmental pollution and global warming and improvement in river water quality. [ABSTRACT FROM AUTHOR]

Published
2022
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90. Burden of influenza in patients with cardiovascular disease who receive antiviral treatment for influenza.

Author

Corral, Mitra, Castro, Rita de Cassia, To, Tu My, Arndorfer, Stella, Wang, Shu, and Stephens, John

Abstract

Cardiovascular disease (CVD) increases the risk of complications from respiratory viruses, including influenza. Moreover, respiratory viruses may increase the risk of CV events. Antiviral medication may reduce healthcare resource utilization (HRU), but more data is needed in CVD populations to explore relationships between influenza antiviral treatment, CVD-related complications, HRU, and costs. This retrospective claims analysis examined data extracted from IBM MarketScan Commercial Claims and Encounters and Medicare Supplemental and Coordination of Benefits databases during three influenza seasons: 2016–2017, 2017–2018, or 2018–2019. Propensity score matching was used to compare HRU outcomes and costs among CVD patients treated with influenza antivirals and untreated patients. Across all influenza seasons, patients with CVD and influenza who received antiviral treatment had fewer all-cause emergency department (ED) visits (p <.01), respiratory-related HRU (p <.01), respiratory-related outpatient and ED visits (both p <.01), CVD-related HRU (p <.01), heart failure-related HRU visits (p <.01), and kidney failure-related HRU (p <.01) 180 days post-treatment fill date than CVD patients untreated for influenza. CVD patients treated with antivirals also had a lower mean number of all-cause inpatient, outpatient, and ED visits and days of stay (all p <.01) and fewer mean respiratory-related outpatient and ED visits (both p <.01). HRU patterns were generally consistent over time and across individual influenza seasons. Finally, treated CVD patients incurred lower all-cause outpatient costs 180 days post-treatment fill date (p <.05) than CVD patients untreated for influenza. CVD patients who contract influenza and take antiviral medication have fewer short- and long-term influenza-related complications and less overall HRU compared with CVD patients who were not prescribed antiviral treatments. Antiviral treatment may be an important tool in reducing complications in CVD patients with influenza. People with heart disease are more likely to have complications from respiratory viruses, including influenza (flu). Moreover, respiratory viruses may increase the risk of damage to the heart muscle. We examined whether patients with heart disease who get the flu and take prescription medications called antiviral drugs have fewer short- and long-term flu-related complications and use fewer healthcare services than patients with heart disease who do not take antiviral drugs. We examined commercial and Medicare databases during three influenza seasons (2016–2017, 2017–2018, and 2018–2019), and we compared outcomes and costs among heart disease patients who were treated or not treated with antiviral drugs. Patients with heart disease and the flu who received antiviral drugs had fewer visits to the emergency room, used fewer healthcare services for respiratory-related problems, used fewer heart disease-related healthcare services, and had fewer heart failure-related or kidney failure-related healthcare visits than heart disease patients who were not treated for the flu. Finally, patients with heart disease who were treated with antiviral drugs spent less money on outpatient services than patients with heart disease who were not treated with antiviral drugs. We determined that patients who get the flu and take antiviral drugs have fewer short- and long-term flu-related complications and use fewer healthcare services than heart disease patients who do not receive antiviral drugs. Therefore, it may be important to treat heart disease patients with antiviral drugs in order to reduce the number of flu-related complications in these patients. [ABSTRACT FROM AUTHOR]

Published
2022
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91. The price tag of a potential cure for chronic hepatitis B infection: A cost threshold analysis for USA, China and Australia.

Author

Toy, Mehlika, Hutton, David, McCulloch, Karen, Romero, Nicole, Revill, Peter A., Penicaud, M‐Capucine, So, Samuel, Cowie, Benjamin C., and Lampertico, Pietro

Subjects
CHRONIC hepatitis B, COST analysis, PRICE marks, HEPATITIS B, VIRUS diseases
Abstract

Background & Aims: We aim to capture the economic impact of a potential cure for chronic hepatitis B infection (CHB) in three countries (USA, China and Australia) with different health systems and epidemics to estimate the threshold drug prices below which a CHB cure would be cost‐saving and/or highly cost‐effective. Methods: We simulated patients' hepatitis B progression, under three scenarios: current long‐term suppressive antiviral therapy, functional cure defined as sustained undetectable HBsAg and HBV DNA, and partial cure defined as sustained undetectable HBV DNA only after a finite, 48‐week treatment. Results: Compared with current long‐term antiviral therapy, a 30% effective functional cure among patients with and without cirrhosis in the USA, China and Australia would yield 17.50, 17.32 and 20.42 QALYs per patient, and 20.61, 20.42 and 20.62 QALYs per patient respectively. In financial terms, for CHB patients with and without cirrhosis, this would be cost‐saving at a one‐time treatment cost under US$11 944 and US$6694, respectively, in the USA, US$1744 and US$1001 in China, and US$12 063 and US$10 983 in Australia. Conclusion: We show that in purely economic terms, a CHB cure will be highly cost‐effective even if effective in only 30% of treated patients. The threshold price for cure is largely determined by the current antiviral drug costs, since it will replace a daily antiviral pill that is inexpensive and effective, although not curative. The likely need for combination therapies to achieve cure will also present cost challenges. While cost‐effectiveness is important, it cannot be the only consideration, as cure will provide many benefits in addition to reduced liver disease and HCC, including eliminating the need for a long‐term daily pill and reducing stigma often associated with chronic viral infection. [ABSTRACT FROM AUTHOR]

Published
2022
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92. Reactive oxygen species as potential antiviral targets.

Author

Sander, Willem J., Fourie, Corinne, Sabiu, Saheed, O'Neill, Frans H., Pohl, Carolina H., and O'Neill, Hester G.

Abstract

Reactive oxygen species (ROS) are by‐products of cellular metabolism and can be either beneficial, at low levels, or deleterious, at high levels, to the cell. It is known that several viral infections can increase oxidative stress, which is mainly facilitated by viral‐induced imbalances in the antioxidant defence mechanisms of the cell. While the exact role of ROS in certain viral infections (adenovirus and dengue virus) remains unknown, other viruses can use ROS for enhancement of pathogenesis (SARS coronavirus and rabies virus) or replication (rhinovirus, West Nile virus and vesicular stomatitis virus) or both (hepatitis C virus, human immunodeficiency virus and influenza virus). While several viral proteins (mainly for hepatitis C and human immunodeficiency virus) have been identified to play a role in ROS formation, most mediators of viral ROS modulation are yet to be elucidated. Treatment of viral infections, including hepatitis C virus, human immunodeficiency virus and influenza virus, with ROS inhibitors has shown a decrease in both pathogenesis and viral replication both in vitro and in animal models. Clinical studies indicating the potential for targeting ROS‐producing pathways as possible broad‐spectrum antiviral targets should be evaluated in randomized controlled trials. [ABSTRACT FROM AUTHOR]

Published
2022
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93. Insights into the Role of Graphene/Graphene‐hybrid Nanocomposites in Antiviral Therapy.

Author

Wu, Xinyun, Manickam, Sivakumar, Wu, Tao, and Pang, Cheng Heng

Subjects
COVID-19, ANTIVIRAL agents, NANOCOMPOSITE materials, DRUG delivery systems, SOCIAL impact, PANDEMICS, ECONOMIC impact
Abstract

The recent coronavirus disease 2019 (COVID‐19) pandemic outbreak has affected the lives of people globally on many different levels. Whilst a few antiviral drugs have been recommended for COVID‐19, there are no dedicated drugs available for this disease, yet. A virus pandemic could potentially induce severe public health threats, as well as economic and social consequences. Therefore, the discovery of effective, safe, and inexpensive antiviral agents is of great importance. Graphene has extraordinary properties. A series of successful biomedical applications involving graphene/graphene‐hybrid nanocomposites (G/GHNs) have been reported in recent years, including graphene‐based biosensor and related drug delivery system. This review is focused on the properties, synthesis routes, and applications of G/GHNs in antiviral therapy aiming to understand and highlight the unique properties of graphene and its derivatives, particularly for antiviral therapy, to evaluate and discuss the quality of graphene prepared via various preparation methods, to present the recent development of G/GHNs and their antiviral activities in prevention, detection and treatment, to offer perspective outlooks on the role of G/GHNs in antiviral therapy. [ABSTRACT FROM AUTHOR]

Published
2021
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94. Hepatitis B virus envelope proteins can serve as therapeutic targets embedded in the host cell plasma membrane.

Author

Zhao, Lili, Chen, Fuwang, Quitt, Oliver, Festag, Marvin, Ringelhan, Marc, Wisskirchen, Karin, Festag, Julia, Yakovleva, Luidmila, Sureau, Camille, Bohne, Felix, Aichler, Michaela, Bruss, Volker, Shevtsov, Maxim, van de Klundert, Maarten, Momburg, Frank, Möhl, Britta S., and Protzer, Ulrike

Subjects
DRUG target, HEPATITIS B virus, VIRAL proteins, CELL membranes, BISPECIFIC antibodies, PLASMA cells
Abstract

Hepatitis B virus (HBV) infection is a major health threat causing 880,000 deaths each year. Available therapies control viral replication but do not cure HBV, leaving patients at risk to develop hepatocellular carcinoma. Here, we show that HBV envelope proteins (HBs)—besides their integration into endosomal membranes—become embedded in the plasma membrane where they can be targeted by redirected T‐cells. HBs was detected on the surface of HBV‐infected cells, in livers of mice replicating HBV and in HBV‐induced hepatocellular carcinoma. Staining with HBs‐specific recombinant antibody MoMab recognising a conformational epitope indicated that membrane‐associated HBs remains correctly folded in HBV‐replicating cells in cell culture and in livers of HBV‐transgenic mice in vivo. MoMab coated onto superparamagnetic iron oxide nanoparticles allowed to detect membrane‐associated HBs after HBV infection by electron microscopy in distinct stretches of the hepatocyte plasma membrane. Last but not least, we demonstrate that HBs located on the cell surface allow therapeutic targeting of HBV‐positive cells by T‐cells either engrafted with a chimeric antigen receptor or redirected by bispecific, T‐cell engager antibodies. Take Aways: HBs become translocated to the plasma membrane.Novel, recombinant antibody confirmed proper conformation of HBs on the membrane.HBs provide an interesting target by T‐cell‐based, potentially curative therapies. [ABSTRACT FROM AUTHOR]

Published
2021
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99. Update on COVID-19 Therapy in Pediatric Age

Author

Susanna Esposito, Giovanni Autore, Alberto Argentiero, Greta Ramundo, Serafina Perrone, and Nicola Principi

Subjects
antiviral therapy, bebtelovimab, COVID-19, molnupiravir, nirmatrelvir/ritonavir, remdesivir, Medicine, Pharmacy and materia medica, RS1-441
Abstract

With the extension of the COVID-19 pandemic, the large use of COVID-19 vaccines among adults and the emergence of SARS-CoV-2 variants means that the epidemiology of COVID-19 in pediatrics, particularly among younger children, has substantially changed. The prevalence of pediatric COVID-19 significantly increased, several severe cases among children were reported, and long-COVID in pediatric age was frequently observed. The main aim of this paper is to discuss which types of treatment are presently available for pediatric patients with COVID-19, which of them are authorized for the first years of life, and which are the most important limitations of COVID-19 therapy in pediatric age. Four different antivirals, remdesivir (RVD), the combination nirmatrelvir plus ritonavir (Paxlovid), molnupiravir (MPV), and the monoclonal antibody bebtelovimab (BEB), are presently approved or authorized for emergency use for COVID-19 treatment by most of the national health authorities, although with limitations according to the clinical relevance of disease and patient’s characteristics. Analyses in the literature show that MPV cannot be used in pediatric age for the risk of adverse events regarding bone growth. The other antivirals can be used, at least in older children, and RDV can be used in all children except in neonates. However, careful research on pharmacokinetic and clinical data specifically collected in neonates and children are urgently needed for the appropriate management of pediatric COVID-19.

Published
2022
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