Bivalent Antiviral Protocol for the Neutralization of Andes Virus (ANDV) and Hantavirus Pulmonary Syndrome (HPS) Date: May 9, 2026 Subject: Emergency Therapeutic Intervention for Interhuman Transmission Clusters Abstract This proposal outlines a dual-phase medical intervention designed to address the high mortality rate and person-to-person transmission of the Andes virus (ANDV). By combining a recombinant Monoclonal Antibody (mAb) cocktail with a targeted RNA-dependent RNA polymerase (RdRp) inhibitor, the protocol seeks to neutralize viral entry while simultaneously halting intracellular replication. This strategy is specifically optimized for high-density environments, such as the May 2026 maritime and cruise-ship outbreaks. 1. Targeted Viral Neutralization The primary therapeutic agent consists of a Human Monoclonal Antibody (mAb) Cocktail (Targeting Gn/Gc Glycoproteins). * Mechanism of Action: The antibodies bind to the viral envelope glycoproteins, physically blocking the virus from attaching to the host’s protocadherin-1 (PCDH1) lung receptors. * Application: Intravenous administration for patients showing early-onset febrile symptoms to prevent the progression to pulmonary edema. 2. Inhibition of Viral Replication To arrest the cytokine storm associated with HPS, a small-molecule Nucleoside Analog (RdRp Inhibitor) is utilized. * Molecular Target: The viral L-protein (RNA-dependent RNA polymerase). * Pharmacodynamics: The inhibitor induces lethal mutagenesis by incorporating fraudulent nucleotides into the viral RNA strand, effectively jamming the replication machinery. * Delivery System: A specialized Nebulized Aerosol delivery to ensure the highest concentration of the inhibitor reaches the pulmonary microvasculature, the primary site of Hantavirus-induced vascular leak. 3. Prophylactic Ring Containment Given the unique human-to-human transmission capability of the Andes strain, the protocol implements a Post-Exposure Prophylaxis (PEP) model: * Tier 1 Exposure: Direct contacts of confirmed cases receive a five-day course of oral inhibitors to prevent viral shedding. * Environmental Control: Deployment of HEPA-filtered laminar flow units in isolation zones to reduce the risk of aerosolized excreta transmission. 4. Clinical Objectives and Mortality Mitigation The protocol aims to reduce the HPS case-fatality rate from the historical ~40% to <5% by addressing the three pillars of the disease: 5. Viremia: Reduced via mAb neutralization. 6. Replication: Halted via RdRp inhibition. 7. Vascular Leak: Managed via integrated JAK/STAT signaling modulation to stabilize capillary permeability. 8. Conclusion The integration of rapid-response diagnostics with bivalent antiviral therapy represents a critical shift in Hantavirus management. This architecture provides a scalable medical framework for containing future zoonotic spillovers and protecting vulnerable populations in confined transit environments. Keywords: Andes Virus (ANDV), Hantavirus Pulmonary Syndrome, RdRp Inhibitors, Monoclonal Antibodies, Viral Neutralization, 2026 Outbreak Response.
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