HIV Mutation Detail Information

Virus Mutation HIV Mutation L363I

Basic Characteristics of Mutations
Mutation Site	L363I
Mutation Site Sentence	To test whether a CA-SP1 cleavage defect can cause HIV-1 to trigger innate sensing, we prepared chimeric VSV-G pseudotyped HIV-1 GFP viruses by transfecting 293T cells with varying ratios of WT HIV-1 GFP and HIV-1 GFP with CA-SP1 Gag mutant L363I M367I (Wiegers et al, 1998;Checkley et al, 2010).
Mutation Level	Amino acid level
Mutation Type	Nonsynonymous substitution
Gene/Protein/Region	Gag
Standardized Encoding Gene	Gag
Genotype/Subtype	HIV-1
Viral Reference	-
Functional Impact and Mechanisms
Disease	HIV Infections
Immune	-
Target Gene	-
Clinical and Epidemiological Correlations
Clinical Information	-
Treatment	-
Location	-
Literature Information
PMID	32852081
Title	Disrupting HIV-1 capsid formation causes cGAS sensing of viral DNA
Author	Sumner RP,Harrison L,Touizer E,Peacock TP,Spencer M,Zuliani-Alvarez L,Towers GJ
Journal	The EMBO journal
Journal Info	2020 Oct 15;39(20):e103958
Abstract	Detection of viral DNA by cyclic GMP-AMP synthase (cGAS) is a first line of defence leading to the production of type I interferon (IFN). As HIV-1 replication is not a strong inducer of IFN, we hypothesised that an intact capsid physically cloaks viral DNA from cGAS. To test this, we generated defective viral particles by treatment with HIV-1 protease inhibitors or by genetic manipulation of gag. These viruses had defective Gag cleavage, reduced infectivity and diminished capacity to saturate TRIM5alpha. Importantly, unlike wild-type HIV-1, infection with cleavage defective HIV-1 triggered an IFN response in THP-1 cells that was dependent on viral DNA and cGAS. An IFN response was also observed in primary human macrophages infected with cleavage defective viruses. Infection in the presence of the capsid destabilising small molecule PF-74 also induced a cGAS-dependent IFN response. These data demonstrate a protective role for capsid and suggest that antiviral activity of capsid- and protease-targeting antivirals may benefit from enhanced innate and adaptive immunity in vivo.
Sequence Data	-

Mutation Information
Note

Basic Characteristics of Mutations

Mutation Site: The specific location in a gene or protein sequence where a change occurs.
Mutation Level: The level at which a mutation occurs, including the nucleotide or amino acid level.
Mutation Type: The nature of the mutation, such as missense mutation, nonsense mutation, synonymous mutation, etc.
Gene/Protein/Region: Refers to the specific region of the virus where the mutation occurs. Including viral genes, viral proteins, or a specific viral genome region. If the article does not specifically indicate the relationship between the mutation and its correspondence, the main
Gene/Protein/Region studied in the article is marked.

Genotype/Subtype: Refers to the viral genotype or subtype where the mutation occurs. If the article does not specifically indicate the relationship between the mutation and its correspondence, the main Genotype/Subtype studied in the article is marked.

Viral Reference: Refers to the standard virus strain used to compare and analyze viral sequences.

Functional Impact and Mechanisms

Disease: An abnormal physiological state with specific symptoms and signs caused by viral infection.

Immune: The article focuses on the study of mutations and immune.

Target Gene: Host genes that viral mutations may affect.

Clinical and Epidemiological Correlations

Clinical Information: The study is a clinical or epidemiological study and provides basic information about the population.

Treatment: The study mentioned a certain treatment method, such as drug resistance caused by mutations. If the study does not specifically indicate the relationship between mutations and their correspondence treatment, the main treatment studied in the article is marked.

Location: The source of the research data.

Literature Information

Sequence Data: The study provides the data accession number.