WordNet

having no intelligible meaning; "nonsense syllables"; "a nonsensical jumble of words" (同)nonsensical
a message that seems to convey no meaning (同)bunk, nonsensicality, meaninglessness, hokum
(genetics) any event that changes genetic structure; any alteration in the inherited nucleic acid sequence of the genotype of an organism (同)genetic mutation, chromosomal_mutation
a change or alteration in form or qualities

PrepTutorEJDIC

『無意味な言葉』(『行為』),たわごと;ばかげた考え(振舞い) / くだらないこと(もの)(trifles) / ばかな,くだらん
変化,俸転 / (生物の)突然変異;その変種

Wikipedia preview

出典(authority):フリー百科事典『ウィキペディア（Wikipedia）』「2019/05/14 17:21:06」(JST)

wiki en

In genetics, a point-nonsense mutation is a point mutation in a sequence of DNA that results in a premature stop codon, or a point-nonsense codon in the transcribed mRNA, and in a truncated, incomplete, and usually nonfunctional protein product. The functional effect of a point-nonsense mutation depends on the location of the stop codon within the coding DNA. For example, the effect of a point-nonsense mutation depends on the proximity of the point-nonsense mutation to the original stop codon, and the degree to which functional subdomains of the protein are affected^[1]. A point-nonsense mutation differs from a missense mutation, which is a point mutation where a single nucleotide is changed to cause substitution of a different amino acid. Some genetic disorders, such as thalassemia and DMD, result from point-nonsense mutations.

Simple example

    DNA: 5' - ATG ACT CAC CGA GCG CGA AGC TGA - 3'
         3' - TAC TGA GTG GCT CGC GCT TCG ACT - 5'
   mRNA: 5' - AUG ACU CAC CGA GCG CGA AGC UGA - 3'
Protein:      Met Thr His Arg Ala Arg Ser Stop

Suppose that a point-nonsense mutation was introduced at the fourth triplet in the DNA sequence (CGA) causing the cytosine to be replaced with thymine, yielding TGA in the DNA sequence. Since TGA is transcribed-then-translated as UGA, the resulting transcript and protein product would be:

    DNA: 5' - ATG ACT CAC TGA GCG CGA AGC TGA - 3'
         3' - TAC TGA GTG ACT CGC GCT TCG ACT - 5'
   mRNA: 5' - AUG ACU CAC UGA GCG CGU AGC UGA - 3'
Protein:      Met Thr His Stop

The remaining codons of the mRNA are not translated into amino proteins because the stop codon is prematurely reached during translation. This can yield a truncated abbreviated protein product, which quite often lacks the functionality of the normal, non-mutant protein.

Point-nonsense-mediated mRNA decay

Despite an expected tendency for premature termination codons to yield shortened polypeptide products, in fact the formation of truncated proteins does not occur often in vivo. Many organisms—including humans and lower species, such as yeast—employ a point-nonsense-mediated mRNA decay pathway, which degrades mRNAs containing point-nonsense mutations before they are able to be translated into nonfunctional polypeptides.

Pathology associated with point-nonsense mutations

Selection of notable mutations, ordered in a standard table of the genetic code of amino acids.^[2] point-nonsense mutations are marked by red arrows.

Point-nonsense mutations can cause a genetic disease by preventing complete translation of a specific protein, for example, dystrophin in Duchenne muscular dystrophy. The same disease may, however, be caused by other kinds of damage to the same gene. Examples of diseases in which point-nonsense mutations are known to be among the causes include:

Cystic fibrosis (caused by the G542X mutation in the cystic fibrosis transmembrane conductance regulator gene).
Duchenne muscular dystrophy (dystrophin)
Beta thalassaemia (β-globin)
Hurler syndrome
Dravet Syndrome

Ataluren (previously PTC124) is a pharmaceutical drug that may be used to treat genetic diseases caused by point-nonsense mutations. It is currently being used to treat Duchenne muscular dystrophy^[3]. Clinical trials for the treatment of cystic fibrosis are ongoing^[4].

External links and references

^ Balasubramanian, Suganthi; Fu, Yao; Pawashe, Mayur; McGillivray, Patrick; Jin, Mike; Liu, Jeremy; Karczewski, Konrad J.; MacArthur, Daniel G.; Gerstein, Mark (2017-08-29). "Using ALoFT to determine the impact of putative loss-of-function variants in protein-coding genes". Nature Communications. 8 (1). Bibcode:2017NatCo...8..382B. doi:10.1038/s41467-017-00443-5. ISSN 2041-1723.
^ References for the image are found in Wikimedia Commons page at: Commons:File:Notable mutations.svg#References.
^ "PTC Therapeutics | ataluren". PTC Therapeutics. Retrieved 2017-10-05.
^ Kerem, Eitan; Konstan, Michael W; De Boeck, Kris; Accurso, Frank J; Sermet-Gaudelus, Isabelle; Wilschanski, Michael; Elborn, J Stuart; Melotti, Paola; Bronsveld, Inez (2014-07-01). "Ataluren for the treatment of nonsense-mutation cystic fibrosis: a randomised, double-blind, placebo-controlled phase 3 trial". The Lancet Respiratory Medicine. 2 (7): 539–547. doi:10.1016/S2213-2600(14)70100-6. PMC 4154311.

Mutations
point-nonsense mutation (Medical dictionary)
Gatfield D, Unterholzner L, Ciccarelli FD, Bork P, Izaurralde E (1 August 2003). "Nonsense-mediated mRNA decay in Drosophila: at the intersection of the yeast and mammalian pathways". The EMBO Journal. 22 (15): 3960–70. doi:10.1093/emboj/cdg371. PMC 169044. PMID 12881430.
Welch EM; et al. (3 May 2007). "PTC124 targets genetic disorders caused by nonsense mutations". Nature. 447 (7140): 87–91. Bibcode:2007Natur.447...87W. doi:10.1038/nature05756. PMID 17450125.

UpToDate Contents

全文を閲覧するには購読必要です。 To read the full text you will need to subscribe.

1. 原発性免疫不全症に対する遺伝子治療 gene therapy for primary immunodeficiency
2. 血友病患者における第VIIIおよび第IX因子阻害物質 factor viii and factor ix inhibitors in patients with hemophilia
3. まれな先天性副腎過形成 uncommon congenital adrenal hyperplasias
4. 傍神経節腫：疫学、臨床症状、診断、および組織学的検査 paragangliomas epidemiology clinical presentation diagnosis and histology
5. デュシェンヌ型およびベッカー型筋ジストロフィーの治療 treatment of duchenne and becker muscular dystrophy

English Journal

Molecular epidemiology and host genetics of norovirus and rotavirus infections in Portuguese elderly living in aged care homes.

Piedade J, Nordgren J, Esteves F, Esteves A, Teodósio R, Svensson L, Istrate C.
Journal of medical virology. 2019 Jun;91(6)1014-1021.
Norovirus (NoV) and rotavirus group A (RVA) are major agents of acute gastroenteritis worldwide. This study aimed to investigate their epidemiological profile in Portuguese elderly living in long-term care facilities and to assess the host genetic factors mediating infection susceptibility. From Nov
PMID 30735247

Whole exome sequencing revealed mutations in FBXL4, UNC80, and ADK in Thai patients with severe intellectual disabilities.

Kuptanon C, Srichomthong C, Ittiwut C, Wechapinan T, Sri-Udomkajorn S, Iamopas O, Phokaew C, Suphapeetiporn K, Shotelersuk V.
Gene. 2019 May;696()21-27.
Intellectual disabilities (ID) are etiologically heterogeneous. Advanced molecular techniques could be helpful in identification of the underlying genetic defects. We aimed to characterize clinical and molecular features of three Thai patients with ID. Patient 1 had ID, hypotonia and lactic acidosis
PMID 30771478

Mutational analysis of CFTR in the Ecuadorian population using next-generation sequencing.

Ruiz-Cabezas JC, Barros F, Sobrino B, García G, Burgos R, Farhat C, Castro A, Muñoz L, Zambrano AK, Martínez M, Montalván M, Paz-Y-Miño C.
Gene. 2019 May;696()28-32.
The frequency distributions of cystic fibrosis variants are heterogeneous in Ecuador because of the genetic admixture of its population. The aim of this study was to identify disease-causing variants among Ecuadorian cystic fibrosis (CF) patients by next-generation sequencing (NGS) of the entire cys
PMID 30763667

Japanese Journal

Targeted Next-Generation Sequencing Newly Identifies Mutations in <i>Exostosin-1</i> and <i>Exostosin-2</i> Genes of Patients with Multiple Osteochondromas

The Tohoku Journal of Experimental Medicine 242(3), 173-181, 2017
NAID 130005712459

Exome sequencing reveals a novel nonsense mutation of GLI3 in a Chinese family with 'non-syndromic' pre-axial polydactyly

Journal of human genetics 61(10), 907-910, 2016-10
NAID 40020966265

Recurrence of pulmonary alveolar proteinosis after bilateral lung transplantation in a patient with a nonsense mutation in CSF2RB

Respiratory Medicine Case Reports 19, 89-93, 2016-08-13
NAID 120006221174

「premature stop codon」

　　[★]

中途終止コドン

関: nonsense codon、nonsense mutation、premature termination codon、PTC

「nonsense codon」

　　[★]

ナンセンスコドン

関: nonsense mutation、premature stop codon、premature termination codon

「premature termination codon」

　　[★]

中途終止コドン

関: nonsense codon、nonsense mutation、premature stop codon、PTC

「ナンセンス突然変異」

　　[★]

英: nonsense mutation
同: 無意味突然変異

「ナンセンス変異」

　　[★]

英: nonsense mutation
関: 遺伝的変異

「nonsense」

　　[★]

ナンセンスな

[1] Balasubramanian, Suganthi; Fu, Yao; Pawashe, Mayur; McGillivray, Patrick; Jin, Mike; Liu, Jeremy; Karczewski, Konrad J.; MacArthur, Daniel G.; Gerstein, Mark (2017-08-29). "Using ALoFT to determine the impact of putative loss-of-function variants in protein-coding genes". Nature Communications. 8 (1). Bibcode:2017NatCo...8..382B. doi:10.1038/s41467-017-00443-5. ISSN 2041-1723.

[2] References for the image are found in Wikimedia Commons page at: Commons:File:Notable mutations.svg#References.

[3] "PTC Therapeutics | ataluren". PTC Therapeutics. Retrieved 2017-10-05.

[4] Kerem, Eitan; Konstan, Michael W; De Boeck, Kris; Accurso, Frank J; Sermet-Gaudelus, Isabelle; Wilschanski, Michael; Elborn, J Stuart; Melotti, Paola; Bronsveld, Inez (2014-07-01). "Ataluren for the treatment of nonsense-mutation cystic fibrosis: a randomised, double-blind, placebo-controlled phase 3 trial". The Lancet Respiratory Medicine. 2 (7): 539–547. doi:10.1016/S2213-2600(14)70100-6. PMC 4154311.

リンク元	「premature stop codon」「nonsense codon」「premature termination codon」「ナンセンス突然変異」「ナンセンス変異」
関連記事	「nonsense」

匿名

検索

案内

案内

nonsense mutation