The Antiviral Effects of Na,K-ATPase Inhibition: A Minireview

Amarelle, Luciano; Lecuona, Emilia

doi:10.3390/ijms19082154

Cited by 54 publications

(53 citation statements)

References 47 publications

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“…In addition to inhibiting HCMV, cardiac glycosides act as antivirals against a range of clinically important DNA and RNA viruses. This broad-spectrum activity has been attributed to a range of host-directed mechanisms [371].…”

Section: Cardiac Glycosidesmentioning

confidence: 99%

Bright and Early: Inhibiting Human Cytomegalovirus by Targeting Major Immediate-Early Gene Expression or Protein Function

Adamson

Nevels

2020

Viruses

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The human cytomegalovirus (HCMV), one of eight human herpesviruses, establishes lifelong latent infections in most people worldwide. Primary or reactivated HCMV infections cause severe disease in immunosuppressed patients and congenital defects in children. There is no vaccine for HCMV, and the currently approved antivirals come with major limitations. Most approved HCMV antivirals target late molecular processes in the viral replication cycle including DNA replication and packaging. “Bright and early” events in HCMV infection have not been exploited for systemic prevention or treatment of disease. Initiation of HCMV replication depends on transcription from the viral major immediate-early (IE) gene. Alternative transcripts produced from this gene give rise to the IE1 and IE2 families of viral proteins, which localize to the host cell nucleus. The IE1 and IE2 proteins are believed to control all subsequent early and late events in HCMV replication, including reactivation from latency, in part by antagonizing intrinsic and innate immune responses. Here we provide an update on the regulation of major IE gene expression and the functions of IE1 and IE2 proteins. We will relate this insight to experimental approaches that target IE gene expression or protein function via molecular gene silencing and editing or small chemical inhibitors.

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Section: Cardiac Glycosidesmentioning

confidence: 99%

Bright and Early: Inhibiting Human Cytomegalovirus by Targeting Major Immediate-Early Gene Expression or Protein Function

Adamson

Nevels

2020

Viruses

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“…Finally, since antiviral properties have been reported for digitoxin and other cardiac glycosides, it is limitation of the study that we cannot exclude other antiviral effects by digitoxin from contributing to the reduction in influenza-dependent cytokine concentration [22][23][24] .…”

Section: Discussionmentioning

confidence: 98%

Classical drug digitoxin inhibits influenza cytokine storm, with implications for COVID-19 therapy

Pollard¹,

Blanco

Pollard

et al. 2020

Preprint

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Influenza viruses, corona viruses and related pneumotropic viruses cause sickness anddeath partly by inducing a hyper-proinflammatory response by immune cells and cytokines in the host airway. Here we show that the cardiac glycoside digitoxin suppresses this response induced by influenza virus strain A/Wuhan/H3N2/359/95 in the cotton rat lung. The cytokines TNFa, GRO/KC, MIP2, MCP1, TGFb, and IFNg. are significantly reduced. Since the hyperproinflammatory overproduction of cytokines is a host response, we suggest that digitoxin may have therapeutic potential for not only influenza and but also for coronovirus infections.

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“…Cohen et al [23] found that the inhibitory activity of cytomegalovirus replication by convallatoxin was due to a decrease in immediate-early gene expression and that the antiviral potency depends on the structure of cardiac glycosides and their specific interactions with Na + / K + -ATPase. It was also shown that influenza virus replication was impaired by ouabain through the inhibition of viral protein translation and a decrease in the intracellular K + concentration [37]. Finally, Boff et al [38] showed that C10 and C11 inhibited Na + /K + -ATPase, and a reduction in intracellular K + concentration could explain the inhibitory activity of those steps of viral infection.…”

Section: Discussionmentioning

confidence: 99%

“…Finally, Boff et al [38] showed that C10 and C11 inhibited Na + /K + -ATPase, and a reduction in intracellular K + concentration could explain the inhibitory activity of those steps of viral infection. In summary, the main antiviral mechanisms suggested for both DNA and RNA viruses are decreased transcription of viral genes and impaired synthesis of viral proteins due to interference with the host translational machinery, such as the inhibition of Na + /K + -ATPase [37]. Structural differences among cardenolides, such as the substituents on the aglycone moiety and the number of sugars, may vary and alter their antiviral activity.…”

Section: Discussionmentioning

confidence: 99%

“…Another suggested possibility is their potential antiviral action, as reported by several authors against adenovirus [18], chikungunya virus [19], coronavirus [20,21], cytomegalovirus [22][23][24], dengue virus [25], herpes virus [26][27][28], HIV [29][30][31], human papillomarivus (HPV) [32], influenza virus [33][34][35], and respiratory syncytial virus [36] replication. The effects of six well-known cardiac glycosides (digoxin, digitoxin, ouabain, convallatoxin, G-strophanthin and lanatoside C) on viral biology and the mechanisms by which they impair the replication of different RNA and DNA viruses were recently compiled [37]. Most of these studies only reported the antiviral activity of cardenolides, and it is required to understand the mechanistic aspects involved and how the compounds really act to further evaluate their potential therapeutic application.…”

Section: Introductionmentioning

confidence: 99%

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Elucidation of the mechanism of anti-herpes action of two novel semisynthetic cardenolide derivatives

et al. 2020

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Human herpesviruses are among the most prevalent pathogens worldwide and have become an important public health issue. Recurrent infections and the emergence of resistant viral strains reinforce the need of searching new drugs to treat herpes virus infections. Cardiac glycosides are used clinically to treat cardiovascular disturbances, such as congestive heart failure and atrial arrhythmias. In recent years, they have sparked new interest in their potential anti-herpes action. It has been previously reported by our research group that two new semisynthetic cardenolides, namely C10 (3β-[(N-(2-hydroxyethyl)aminoacetyl] amino-3-deoxydigitoxigenin) and C11 (3β-(hydroxyacetyl)amino-3-deoxydigitoxigenin), exhibited potential anti-HSV-1 and anti-HSV-2 with selectivity index values > 1,000, comparable with those of acyclovir. This work reports the mechanism investigation of anti-herpes action of these derivatives. The results demonstrated that C10 and C11 interfere with the intermediate and final steps of HSV replication, but not with the early stages, since they completely abolished the expression of the UL42 (β) and gD (γ) proteins and partially reduced that of ICP27 (α). Additionally, they were not virucidal and had no prophylactic effects. Both compounds inhibited HSV replication at nanomolar concentrations, but cardenolide C10 was more active than C11 and can be considered as an anti-herpes drug candidate including against acyclovir-resistant HSV-1 strains. AbbreviationsACV acyclovir CC 50 50% cytotoxic concentration CMC carboxymethylcellulose DEX-S dextran sulfate FBS fetal bovine serum HIV human immunodeficiency virus HSV-1 herpes simplex virus type 1 HSV-2 herpes simplex virus type 2 HPV human papillomavirus IC 50 concentration that inhibited 50% of viral replication MEM Eagle's minimum essential medium MOI multiplicity of infection PBS phosphate-buffered saline PFU plaque-forming units SI selectivity index

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The Antiviral Effects of Na,K-ATPase Inhibition: A Minireview

Cited by 54 publications

References 47 publications

Bright and Early: Inhibiting Human Cytomegalovirus by Targeting Major Immediate-Early Gene Expression or Protein Function

Bright and Early: Inhibiting Human Cytomegalovirus by Targeting Major Immediate-Early Gene Expression or Protein Function

Classical drug digitoxin inhibits influenza cytokine storm, with implications for COVID-19 therapy

Elucidation of the mechanism of anti-herpes action of two novel semisynthetic cardenolide derivatives

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