Table 2.
List of drugs having clinical effectiveness in COVID-19 therapy targeting various targets of SARS-CoV-2.
| S. No. | Drug | Use | Target | Mechanism of action | Clinical trial | Ref. |
|---|---|---|---|---|---|---|
| 1 | Atazanavir | HIV | SARS-CoV-2 Mpro | Atazanavir could adjust in Mpro active site and can I inhibit its activity resulting in a disruption in viral replication. | Phase 2: NCT04459286 | [64] |
| 2 | Baricitinib | Rheumatoid arthritis | Human AP2-associated protein kinase 1 (AAK1); Janus kinase (JAK) 1 and 2 | Can block the entry and infectivity of SARS CoV-2 in pneumocytes by impairing AAK1 that are involved in virus endocytosis; also inhibit the intracellular signaling pathway of cytokines IL-2, 6, 10 and INF-γ, a granulocyte-macrophage colony-stimulating factor that is enhanced in severe SARS CoV-2 infection | Phase 2: NCT04321993; Phases 2 and 3: NCT04320277; Phase 3 NCT04421027 |
[[65], [66], [67]] |
| 3 | Mefuparib hydrochloride (CVL218) | Cancer | N protein; poly-ADP-ribose polymerase 1(PARP1) | Can target N protein to reduce its RNA binding and thus impede viral replication; inhibit the production of IL-6 by CpG oligodeoxynucleotide 1826 in peripheral blood mononuclear cells | Phase 1 | [68] |
| 4 | Pemirolast, nitrofurantoin isoniazid pyruvate, eriodictyol | Numerous | ACE2 receptor | Can interact with ACE2 receptor more efficiently and inhibit undesirable S protein to ACE2 interaction. | – | [69] |
| 5 | Cepharanthine, ergoloid, hypericin | Numerous | S protein | Can cause favorable ring-protein interaction which blocks host recognition | – | [69] |
| 6 | Remdesivir | Ebola | RdRP | Nucleoside (adenosine) analogue RdRP inhibitor which inhibits RNA synthesis and can result in premature termination | Phase 3: NCT04292899 | [70,71] |
| 7 | Chloroquine/hydroxychloroquine | Malaria, lupus and rheumatoid arthritis | Affect both early and late stage of viral replication | keep the virus out of host cells by disturbing ACE2 glycosylation and breaking down the production of viral proteins by inhibiting endosomal acidification. | Phase 2 and 3: NCT04353336 | [70,72,[74], [75], [76]] |
| 8 | Lopinavir/ritonavir combination | HIV | 3CLpro | Disrupt the process of viral replication and release from the cell. | Phase 2: NCT0427668 | [77,78] |
| 9 | Nafamostat or camostat | Pancreatitis | Serine protease TMPRSS2 | Acts as an antagonist to the serine protease TMPRSS2; Prevents membrane fusion by reducing the release of cathepsin B. | Phase 2 and 3: NCT04418128 Phase 2: NCT04625114 | [79] |
| 10 | Famotidine | Heartburn | PLpro | Possibly bind PLpro which is known to be essential to the entry of SARS-CoV-2 | Phase 3: NCT04504240 | [80] |
| 11 | Umifenovir | Influenza | Viral lipid membrane | Can bind viral lipid membrane and affect cellular trafficking of the virus | Phase 4: NCT04350684 | [81] |
| 12 | Nitazoxanide | Influenza; diarrhoea | Not known | Can suppress maturation of the viral hemagglutinin and the viral transcription factor immediate-early 2 (IE2) as well as by activating the translation INF2α. | Phase 2: NCT04552483 | [82] |
| 13 | Ivermectin | Influenza; dengue; broad-spectrum antiparasitic | Not known | Can inhibit expression of the viral N protein and IL-6; Inhibit viral IMPα/β1-mediated nuclear import, causing a reduction in viral replication; Can also work by binding and destabilizing cell-transport proteins used to enter the nucleus. | Phase 1: NCT04343092 | [83] |
| 14 | Teicoplanin | Gram-positive bacterial infection | Not known | Inhibit the activity of cathepsin L which potentially plays an important role in blocking viral entry in the cells | – | [84] |
| 15 | Tocilizumab/sarilumab (mAb) | Rheumatoid arthritis | IL-6 receptor antagonists | Inhibition of IL-6 may attenuate pulmonary inflammation and fibrosis | Phase 3 and Phase 2/3: NCT04315298 | [84] |
| 16 | Anti TNF-α agents | Rheumatoid arthritis | TNF-α | TNF-α blockage leads to down-regulation of pro-inflammatory mediators, including IL-1, IL-6, and granulocyte-macrophage colony-stimulating factor as well as cytokines and acute-phase proteins | – | [84] |