Genetic Instabilities in (CTG.CAG) Repeats Occur by Recombination
Overview
Authors
Affiliations
The expansion of triplet repeat sequences (TRS) associated with hereditary neurological diseases is believed from prior studies to be due to DNA replication. This report demonstrates that the expansion of (CTG.CAG)(n) in vivo also occurs by homologous recombination as shown by biochemical and genetic studies. A two-plasmid recombination system was established in Escherichia coli with derivatives of pUC19 (harboring the ampicillin resistance gene) and pACYC184 (harboring the tetracycline resistance gene). The derivatives contained various triplet repeat inserts ((CTG.CAG), (CGG.CCG), (GAA.TTC), (GTC.GAC), and (GTG.CAC)) of different lengths, orientations, and extents of interruptions and a control non-repetitive sequence. The availability of the two drug resistance genes and of several unique restriction sites on the plasmids enabled rigorous genetic and biochemical analyses. The requirements for recombination at the TRS include repeat lengths >30, the presence of CTG.CAG on both plasmids, and recA and recBC. Sequence analyses on a number of DNA products isolated from individual colonies directly demonstrated the crossing-over and expansion of the homologous CTG.CAG regions. Furthermore, inversion products of the type [(CTG)(13)(CAG)(67)].[(CTG)(67)(CAG)(13)] were isolated as the apparent result of "illegitimate" recombination events on intrahelical pseudoknots. This work establishes the relationships between CTG.CAG sequences, multiple fold expansions, genetic recombination, formation of new recombinant DNA products, and the presence of both drug resistance genes. Thus, if these reactions occur in humans, unequal crossing-over or gene conversion may also contribute to the expansions responsible for anticipation associated with several hereditary neurological syndromes.
Mosaicism in Short Tandem Repeat Disorders: A Clinical Perspective.
Doss R, Lopez-Ignacio S, Dischler A, Hiatt L, Dashnow H, Breuss M Genes (Basel). 2025; 16(2).
PMID: 40004546 PMC: 11855715. DOI: 10.3390/genes16020216.
Genome-wide identification and characterization of microsatellite markers within the Avipoxviruses.
Sahu B, Majee P, Singh R, Sahoo N, Nayak D 3 Biotech. 2022; 12(5):113.
PMID: 35497507 PMC: 9008116. DOI: 10.1007/s13205-022-03169-4.
Yao D, Cheng L, Du L, Li M, Daroch M, Tang J Life (Basel). 2021; 11(11).
PMID: 34833134 PMC: 8619395. DOI: 10.3390/life11111258.
Borne R, Vita N, Franche N, Tardif C, Perret S, Fierobe H Metab Eng Commun. 2021; 12:e00157.
PMID: 33457204 PMC: 7797564. DOI: 10.1016/j.mec.2020.e00157.
The Need for Establishing a Universal CTG Sizing Method in Myotonic Dystrophy Type 1.
Ballester-Lopez A, Linares-Pardo I, Koehorst E, Nunez-Manchon J, Pintos-Morell G, Coll-Canti J Genes (Basel). 2020; 11(7).
PMID: 32645888 PMC: 7397178. DOI: 10.3390/genes11070757.