PMID-sentid	Pub_year	Sent_text		comp_official_name	comp_offsetprotein_name	organism	prot_offset
34052981-0	2021	The application of in silico experimental model in the assessment of ciprofloxacin and levofloxacin interaction with main SARS-CoV-2 targets: S-, E- and TMPRSS2 proteins, RNA-dependent RNA polymerase and papain-like protease (PLpro)-preliminary molecular docking analysis.	Levofloxacin	87-99	transmembrane serine protease 2	Homo sapiens	153-160	
34052981-3	2021	METHODS: In the present study molecular docking technique was applied to test binding affinity of ciprofloxacin and levofloxacin-two commercially available fluoroquinolones, to SARS-CoV-2 S-, E- and TMPRSS2 proteins, RNA-dependent RNA polymerase and papain-like protease (PLPRO).	Levofloxacin	116-128	transmembrane serine protease 2	Homo sapiens	199-206	
34052981-6	2021	In the case of TMPRSS2 protein and PLPRO protease the best docked ligand was levofloxacin and in the case of E proteins and RNA-dependent RNA polymerase the best docked ligands were levofloxacin and dexamethasone.	Levofloxacin	77-89	transmembrane serine protease 2	Homo sapiens	15-22	
34052981-7	2021	Moreover, a molecular dynamics study also reveals that ciprofloxacin and levofloxacin form a stable complex with E- and TMPRSS2 proteins, RNA polymerase and papain-like protease (PLPRO).	Levofloxacin	73-85	transmembrane serine protease 2	Homo sapiens	120-127