What Is 3-chymotrypsin-like protease

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Last updated: April 15, 2026

Quick Answer: 3-chymotrypsin-like protease (3CLpro), also known as main protease (Mpro), is a key enzyme in the replication of coronaviruses, including SARS-CoV-2, first identified in 2003 during the SARS outbreak. It cleaves viral polyproteins at 11+ specific sites to enable functional protein assembly, making it a prime target for antiviral drugs like Paxlovid.

Key Facts

3CLpro was first identified in the SARS-CoV virus in 2003
It cleaves viral polyproteins at 11 or more specific sites
The enzyme's active site recognizes leucine, phenylalanine, or tryptophan at the P1 position
Paxlovid, approved in 2021, inhibits 3CLpro to treat COVID-19
3CLpro has no close human homologs, reducing risk of side effects

Overview

3-chymotrypsin-like protease (3CLpro), also known as the main protease (Mpro), is a critical enzyme in the life cycle of coronaviruses such as SARS-CoV, MERS-CoV, and SARS-CoV-2. It plays a central role in processing viral polyproteins into functional units necessary for replication and assembly of new viral particles.

Discovered during the 2003 SARS outbreak, 3CLpro has since become a major focus of antiviral drug development due to its essential function and structural uniqueness. Unlike many viral enzymes, it has no close human equivalent, making it an ideal target for selective inhibition.

First identified in 2003: Researchers isolated and characterized 3CLpro during the original SARS-CoV outbreak, marking a pivotal moment in coronavirus enzymology.
Essential for viral replication: Without 3CLpro, the virus cannot process its polyproteins, halting the production of infectious virions within infected cells.
Highly conserved across coronaviruses: The enzyme’s sequence and structure remain similar across different coronaviruses, enabling broad-spectrum drug design.
Composed of 306 amino acids: In SARS-CoV-2, the 3CLpro enzyme forms a homodimer, with each monomer contributing to the active site.
Crystal structure solved by 2005: X-ray crystallography revealed its 3D structure, enabling structure-based drug discovery efforts worldwide.

How It Works

3CLpro functions by cleaving peptide bonds at specific locations in the viral polyprotein chain, releasing non-structural proteins essential for replication. Its specificity and efficiency make it indispensable to the virus’s life cycle.

Autocleavage:3CLpro initially cleaves itself from the polyprotein chain, a self-processing step that activates its enzymatic function within hours of infection.
Substrate specificity:The enzyme recognizes a conserved sequence ending in glutamine at the P1 position, with high selectivity for leucine, phenylalanine, or tryptophan at P2.
Catalytic dyad:Uses residues His41 and Cys145 to form a catalytic dyad that performs nucleophilic attack on peptide bonds, distinguishing it from human serine proteases.
Dimerization:Functional 3CLpro exists as a dimer, where two identical subunits interact to stabilize the active site and enhance enzymatic efficiency.
Replication complex role:Operates within the viral replication-transcription complex, processing up to 16 cleavage sites in the polyprotein to release functional enzymes like RNA-dependent RNA polymerase.
Inhibition mechanism:Drugs like nirmatrelvir in Paxlovid bind covalently to Cys145, blocking the active site and preventing further cleavage activity.

Comparison at a Glance

Below is a comparison of 3CLpro across major human-infecting coronaviruses:

Virus	Year Identified	Sequence Identity	Drug Target?	Known Inhibitors
SARS-CoV	2003	96%	Yes	Lopinavir, GC376
SARS-CoV-2	2019	100%	Yes	Nirmatrelvir (Paxlovid)
MERS-CoV	2012	49%	Yes	Boceprevir
HCoV-229E	1960s	44%	Experimental	None approved
HCoV-OC43	1967	52%	Experimental	Preclinical candidates

The high degree of conservation in 3CLpro across strains supports the development of pan-coronavirus inhibitors. While SARS-CoV-2 shares nearly identical active site geometry with SARS-CoV, MERS-CoV diverges more significantly, requiring tailored drug approaches. Despite differences, all rely on 3CLpro for polyprotein processing, validating it as a universal antiviral target.

Why It Matters

Understanding 3CLpro has direct implications for public health, especially in pandemic preparedness and antiviral therapy. Its role in viral replication and lack of human analogs make it a safe and effective drug target.

Paxlovid approval in 2021: The FDA authorized nirmatrelvir/ritonavir, a 3CLpro inhibitor, for emergency use, reducing hospitalization by 89% in high-risk patients.
Broad-spectrum potential: Drugs targeting 3CLpro could be effective against future zoonotic coronaviruses due to the enzyme’s evolutionary stability.
Low risk of off-target effects: Humans lack a close homolog of 3CLpro, minimizing the chance of adverse reactions from inhibitors.
Resistance monitoring: Emerging mutations in 3CLpro, such as E166V, are being tracked to ensure long-term drug efficacy.
Cost-effective treatment: Oral 3CLpro inhibitors like Paxlovid offer outpatient management, reducing strain on healthcare systems.
Foundation for next-gen antivirals: Research on 3CLpro informs the design of covalent inhibitors, prodrugs, and combination therapies for future outbreaks.

As coronaviruses continue to pose global health threats, 3CLpro remains a cornerstone of antiviral research. Its well-defined mechanism and druggability offer a proven path for rapid response in future pandemics.