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α-ketoamide 13b for COVID-19

α-ketoamide 13b has been reported as potentially beneficial for treatment of COVID-19. We have not reviewed these studies. See all other treatments.
Kumar et al., In Silico Identification and Docking-Based Drug Repurposing Against the Main Protease of SARS-CoV-2, Causative Agent of COVID-19, American Chemical Society (ACS), doi:10.26434/chemrxiv.12049590.v1
The rapidly enlarging COVID-19 pandemic caused by novel SARS-coronavirus 2 is a globalpublic health emergency of unprecedented level. Therefore the need of a drug or vaccine thatcounter SARS-CoV-2 is an utmost requirement at this time. Upon infection the ssRNA genomeof SARS-CoV-2 is translated into large polyprotein which further processed into differentnonstructural proteins to form viral replication complex by virtue of virus specific proteases:main protease (3-CL protease) and papain protease. This indispensable function of main proteasein virus replication makes this enzyme a promising target for the development of inhibitors andpotential treatment therapy for novel coronavirus infection. The recently concluded α-ketoamideligand bound X-ray crystal structure of SARS-CoV-2 Mpro (PDB ID: 6Y2F) from Zhang et al.has revealed the potential inhibitor binding mechanism and the determinants responsible forinvolved molecular interactions. Here, we have carried out a virtual screening and moleculardocking study of FDA approved drugs primarily targeted for other viral infections, to investigatetheir binding affinity in Mpro active site. Virtual screening has identified a number of antiviraldrugs, top ten of which on the basis of their bending energy score are further examined through molecular docking with Mpro. Docking studies revealed that drug Lopinavir-Ritonavir, Tipranavirand Raltegravir among others binds in the active site of the protease with similar or higheraffinity than the crystal bound inhibitor α-ketoamide. However, the in-vitro efficacies of the drugmolecules tested in this study, further needs to be corroborated by carrying out biochemical andstructural investigation. Moreover, this study advances the potential use of existing drugs to beinvestigated and used to contain the rapidly expanding SARS-CoV-2 infection.
Tam et al., Targeting SARS-CoV-2 Non-Structural Proteins, International Journal of Molecular Sciences, doi:10.3390/ijms241613002
Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is an enveloped respiratory β coronavirus that causes coronavirus disease (COVID-19), leading to a deadly pandemic that has claimed millions of lives worldwide. Like other coronaviruses, the SARS-CoV-2 genome also codes for non-structural proteins (NSPs). These NSPs are found within open reading frame 1a (ORF1a) and open reading frame 1ab (ORF1ab) of the SARS-CoV-2 genome and encode NSP1 to NSP11 and NSP12 to NSP16, respectively. This study aimed to collect the available literature regarding NSP inhibitors. In addition, we searched the natural product database looking for similar structures. The results showed that similar structures could be tested as potential inhibitors of the NSPs.
Please send us corrections, updates, or comments. c19early involves the extraction of 100,000+ datapoints from thousands of papers. Community updates help ensure high accuracy. Treatments and other interventions are complementary. All practical, effective, and safe means should be used based on risk/benefit analysis. No treatment or intervention is 100% available and effective for all current and future variants. We do not provide medical advice. Before taking any medication, consult a qualified physician who can provide personalized advice and details of risks and benefits based on your medical history and situation. FLCCC and WCH provide treatment protocols.
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