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Mitochondrial Variants

This code was designed to create a table of mitochondrial variants, their associated amino acid changes (if any), which features these changes affect, predicted consequences (with SIFT and PolyPhen scores), associated diseases, and the frequency of these variants in the general population. Sources for this information include Ensembl Variant Effect Predictor, MitoMap, and GenomeNet.

Code:

  • revision_code.R — used to create the final output file, rev_table.txt

Input Files:

Output Files:

  • variant_table.txt — all possible variants in the mitochondrial genome (single substitution, no insertion or deletion). Used as input for VEP

  • VEP_redu.txt — intermediate table, prior to integration with MitoMap information

  • rev_table.txt — final output table

Final Output Description:

  1. Position — 1-16569 bp. The total number of possible variants is 3x16,569+1=49,708 because the mitochondrial genome (NC_012920) is 16,569 bp with three possible variants each, except base 3,107, which has four possible variants (A, C, T, G) because the reference is N. You will notice that there are not the expected 49,708 rows but instead a few hundred more. This is because sometimes more than one gene is associated with the same position and therefore it receives multiple lines
  2. Reference — reference nucleotide from https://www.genome.jp/dbget-bin/www_bget?-f+refseq+NC_012920
  3. Variant — each possible variant, 3 for all positions with the exception of 3,107, which has 4
  4. Consequence — (VEP) predicted consequence of the variant
  5. Symbol — (VEP) gene symbol
  6. Gene — (VEP) Ensembl gene ID
  7. Feature type — (VEP) type of feature affected: transcript, regulatory feature, or motif feature
  8. Feature — (VEP) Ensembl transcript ID or other identifier, based on feature type
  9. Biotype — (VEP) type of transcript or regulatory feature: protein coding, tRNA, or rRNA. More are present in VEP but not associated with mitochondria
  10. Amino acids — (VEP) any amino acid changes that occur due to the variant
  11. Codons — (VEP) if an amino acid change occurs, this is shows which codon was changed, with the affected nucleotide in the capital letter
  12. SIFT — (VEP) SIFT prediction score for whether an amino acid change will affect protein function (https://www.ncbi.nlm.nih.gov/pmc/articles/PMC168916/)
  13. PolyPhen — (VEP) PolyPhen prediction score for whether an amino acid change will affect protein function (https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4480630/)
  14. Homoplasmy* — (MitoMap)
  15. Heteroplasmy* — (MitoMap)
  16. Disease* — (MitoMap) diseases associated with a particular variant
  17. Status* — (MitoMap) has this variant been reported or confirmed?
  18. GB Count — (MitoMap) GenBank count
  19. GB Frequency — (MitoMap) GenBank frequency. See the following for more information on columns 18 and 19 (https://www.mitomap.org/MITOMAP/GBFreqInfo)

NOTE: Any cells containing "-" are unknown values, and should be treated as distinct from zero values in the table.

Notes for the (*) indicated columns (from MitoMap):

  • LHON — Leber Hereditary Optic Neuropathy
  • MM — Mitochondrial Myopathy
  • AD — Alzeimer's Disease
  • LIMM — Lethal Infantile Mitochondrial Myopathy
  • ADPD — Alzeimer's Disease and Parkinsons's Disease
  • MMC — Maternal Myopathy and Cardiomyopathy
  • NARP — Neurogenic muscle weakness, Ataxia, and Retinitis Pigmentosa; alternate phenotype at this locus is reported as Leigh Disease
  • FICP — Fatal Infantile Cardiomyopathy Plus, a MELAS-associated cardiomyopathy
  • MELAS — Mitochondrial Encephalomyopathy, Lactic Acidosis, and Stroke-like episodes
  • LDYT — Leber's hereditary optic neuropathy and DYsTonia
  • MERRF — Myoclonic Epilepsy and Ragged Red Muscle Fibers
  • MHCM — Maternally inherited Hypertrophic CardioMyopathy
  • CPEO — Chronic Progressive External Ophthalmoplegia
  • KSS — Kearns Sayre Syndrome
  • DM – Diabetes Mellitus
  • DMDF — Diabetes Mellitus + DeaFness
  • CIPO — Chronic Intestinal Pseudoobstruction with myopathy and Ophthalmoplegia
  • DEAF — Maternally inherited DEAFness or aminoglycoside-induced DEAFness
  • PEM — Progressive encephalopathy
  • SNHL — SensoriNeural Hearing Loss

** Homoplasmy = pure mutant mtDNAs.

** Heteroplasmy = mixture of mutant and normal mtDNAs.

** nd = not determined.

** "Reported" status indicates that one or more publications have considered the mutation as possibly pathologic. This is not an assignment of pathogenicity by MITOMAP but is a report of literature. Previously, mutations with this status were termed "Prov" (provisional).

** "Cfrm"(confirmed) status indicates that at least two or more independent laboratories have published reports on the pathogenicity of a specific mutation. These mutations are generally accepted by the mitochondrial research community as being pathogenic. A status of "Cfrm" is not an assignment of pathogenicity by MITOMAP but is a report of published literature. Researchers and clinicians are cautioned that additional data and/or analysis may still be necessary to confirm the pathological significance of some of these mutations.

** "P.M." (point mutation / polymorphism) status indicates that some published reports have determined the mutation to be a non-pathogenic polymorphism.

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