inst/markdown/methods/neoantigen-classes.markdown
In CRI-iAtlas/iatlas-app: What the Package Does (One Line, Title Case)
Title: Classes of predicted neoantigens
Description:
The classes of neoantigens predicted by LENS are:
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Somatic SNVs: Somatic single-nucleotide variants (SNVs), or variants present within tumor tissue but absent from germline tissue. These peptides may be a direct result of a somatic variant or may be a downstream coding consequence of the variant.
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Somatic InDels: Somatic insertion/deletion variants (InDels), or variants present within tumor tissue but absent from germline tissue. These peptides may be a direct result of a somatic variant or may be a downstream coding consequence of the variant.
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Fusion Events: Scenarios in which a translocation, deletion, or inversion causes two previously genomically distant loci to become neighboring sequences or “fuse” within the genome are also of interest as sources of tumor antigens.
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Splice Variants: Aberrant splicing events create tumor-specific transcripts through intron retention, exon skipping, or altered splice targeting.
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CTAs and Self-antigens: These antigens are non-mutated self-antigens that may be overexpressed within a tumor. Antigens derived from these transcripts are commonly referred to as cancer testis antigens (CTAs).
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Virus: Some viruses, such as human papillomavirus, Epstein–Barr virus, human T cell leukemia/lymphoma virus type 1, and hepatitis C virus, are associated with development of cancers in the tissues they infect earning them the label of oncogenic viruses.
-
ERVs: Aberrantly expressed endogenous retroviruses (ERVs).
More information about LENS is available at:
Contributors: Steven P Vensko II, Dante Bortone, Carolina Heimann
CRI-iAtlas/iatlas-app documentation built on Feb. 7, 2025, 9:02 p.m.
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Title: Classes of predicted neoantigens
Description: The classes of neoantigens predicted by LENS are:
-
Somatic SNVs: Somatic single-nucleotide variants (SNVs), or variants present within tumor tissue but absent from germline tissue. These peptides may be a direct result of a somatic variant or may be a downstream coding consequence of the variant.
-
Somatic InDels: Somatic insertion/deletion variants (InDels), or variants present within tumor tissue but absent from germline tissue. These peptides may be a direct result of a somatic variant or may be a downstream coding consequence of the variant.
-
Fusion Events: Scenarios in which a translocation, deletion, or inversion causes two previously genomically distant loci to become neighboring sequences or “fuse” within the genome are also of interest as sources of tumor antigens.
-
Splice Variants: Aberrant splicing events create tumor-specific transcripts through intron retention, exon skipping, or altered splice targeting.
-
CTAs and Self-antigens: These antigens are non-mutated self-antigens that may be overexpressed within a tumor. Antigens derived from these transcripts are commonly referred to as cancer testis antigens (CTAs).
-
Virus: Some viruses, such as human papillomavirus, Epstein–Barr virus, human T cell leukemia/lymphoma virus type 1, and hepatitis C virus, are associated with development of cancers in the tissues they infect earning them the label of oncogenic viruses.
-
ERVs: Aberrantly expressed endogenous retroviruses (ERVs).
More information about LENS is available at:
Contributors: Steven P Vensko II, Dante Bortone, Carolina Heimann
R Package Documentation
Browse R Packages
We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
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