Recapitulation of gametic DNA methylation and its post-fertilization maintenance with reassembled DNA elements at the mouse Igf2/H19 locus

Matsuzaki, Hitomi; Kuramochi, Daichi; Okamura, Eiichi; Hirakawa, Katsuhiko; Ushiki, Aki; Tanimoto, Koichi

doi:10.1186/s13072-019-0326-1

Cited by 11 publications

(11 citation statements)

References 34 publications

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“…As mentioned earlier, we identified the 118-bp sequence that is essential for post-fertilization imprinted methylation of the mouse H19 ICR during the preimplantation period [17,18,27]. We further demonstrated that this sequence, together with the CTCF and Sox/Oct binding sequences, could confer imprinted methylation activity to the non-imprinted lambda DNA sequence both in transgenic [27] and endogenous genomic contexts [28].…”

Section: Introductionsupporting

confidence: 62%

“…Since mIG-DMR analyzed at the same genomic location exhibited post-fertilization imprinted methylation, it is unlikely that the results in the rat sequence are related to the insertion site of the transgene. In addition, our previous reconstruction experiments showed differential methylation of the LCb118 fragment, in which the CTCF, Sox/Oct, and Zfp57 motifs were embedded in lambda DNA in the same context as the mouse H19 ICR and then combined with the mouse 118-bp sequence [28]. Because binding sequences for these factors are highly conserved in number and arrangement between mouse and rat H19 ICRs (Additional file 1: Fig.…”

Section: Discussionmentioning

confidence: 99%

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The transgenic IG-DMR sequence of the mouse Dlk1-Dio3 domain acquired imprinted DNA methylation during the post-fertilization period

Matsuzaki

Sugihara

Tanimoto

2023

Epigenetics & Chromatin

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Background Allele-specific methylation of the imprinting control region (ICR) is the molecular basis for the genomic imprinting phenomenon that is unique to placental mammals. We previously showed that the ICR at the mouse H19 gene locus (H19 ICR) was unexpectedly established after fertilization and not during spermatogenesis in transgenic mice (TgM), and that the same activity was essential for the maintenance of paternal methylation of the H19 ICR at the endogenous locus in pre-implantation embryos. To examine the universality of post-fertilization imprinted methylation across animal species or imprinted loci, we generated TgM with two additional sequences. Results The rat H19 ICR, which is very similar in structure to the mouse H19 ICR, unexpectedly did not acquire imprinted methylation even after fertilization, suggesting a lack of essential sequences in the transgene fragment. In contrast, the mouse IG-DMR, the methylation of which is acquired during spermatogenesis at the endogenous locus, did not acquire methylation in the sperm of TgM, yet became highly methylated in blastocysts after fertilization, but only when the transgene was paternally inherited. Since these two sequences were evaluated at the same genomic site by employing the transgene co-placement strategy, it is likely that the phenotype reflects the intrinsic activity of these fragments rather than position-effect variegation. Conclusions Our results suggested that post-fertilization imprinted methylation is a versatile mechanism for protecting paternal imprinted methylation from reprogramming during the pre-implantation period.

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Section: Introductionsupporting

confidence: 62%

Section: Discussionmentioning

confidence: 99%

The transgenic IG-DMR sequence of the mouse Dlk1-Dio3 domain acquired imprinted DNA methylation during the post-fertilization period

Matsuzaki

Sugihara

Tanimoto

2023

Epigenetics & Chromatin

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“…Indeed, following polyspermic fertilization, where methylation of the maternal genome remains relatively constant, up to five paternal genomes are demethylated in the zygote 4 . Although zygotic de novo DNAme of the maternal genome has been reported for the TKZ751 transgene and Igf2 59 , ETn retroelements 60 and H3K9me2-enriched regions 61 , to our knowledge, this is the first report to identify specific regions of the paternal genome subject to de novo DNAme by the 2C stage beyond the H19 gDMR 46 , 62 , 63 .…”

Section: Discussionmentioning

confidence: 76%

Maternal DNMT3A-dependent de novo methylation of the paternal genome inhibits gene expression in the early embryo

et al. 2020

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De novo DNA methylation (DNAme) during mammalian spermatogenesis yields a densely methylated genome, with the exception of CpG islands (CGIs), which are hypomethylated in sperm. While the paternal genome undergoes widespread DNAme loss before the first S-phase following fertilization, recent mass spectrometry analysis revealed that the zygotic paternal genome is paradoxically also subject to a low level of de novo DNAme. However, the loci involved, and impact on transcription were not addressed. Here, we employ allele-specific analysis of whole-genome bisulphite sequencing data and show that a number of genomic regions, including several dozen CGI promoters, are de novo methylated on the paternal genome by the 2-cell stage. A subset of these promoters maintains DNAme through development to the blastocyst stage. Consistent with paternal DNAme acquisition, many of these loci are hypermethylated in androgenetic blastocysts but hypomethylated in parthenogenetic blastocysts. Paternal DNAme acquisition is lost following maternal deletion of Dnmt3a, with a subset of promoters, which are normally transcribed from the paternal allele in blastocysts, being prematurely transcribed at the 4-cell stage in maternal Dnmt3a knockout embryos. These observations uncover a role for maternal DNMT3A activity in post-fertilization epigenetic reprogramming and transcriptional silencing of the paternal genome.

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“…Two-fold rise for Igf2 gene (strongly linked to spermatogenesis, sex determination, testis development, infertility and prostate cancer; [Matsuzaki et al , 2020; Cannarella et al , 2020; Neirijnck et al , 2019; Damaschke et al , 2017]) has been also noticed. Igf2 and Klk proteins are enclosed in a common network consisted of proteins directly linked to fertility (Figure 6; Supplementary file 11; Supplementary file 12).…”

Section: Resultsmentioning

confidence: 99%

“…Our pathway analysis revealed a network including two genes with changed expression level in testis: Igf2 (2-fold increased) and Klk1b22 (8-fold decreased), supported by an interesting set of proteins linked to apoptosis and cellular processing (Figure 5; Figure 6; Supplementary file 11; Supplementary file 12). We can suggest that observed Igf2 overexpression in our study can be one of the associated factors leading to decreased sperm count and testis parameters in evaluated KO mice model because of its known relation to spermatogenesis and testis development [Matsuzaki et al , 2020; Cannarella et al , 2020; Neirijnck et al , 2019; Damaschke et al , 2017]. Documented reductions can be supported by the observed constrained expression of Klk1b22 – kallikrein mostly known from its neuronal activity; however, it cannot be excluded that we have revealed additional role of this protein, similar to the other members of the kallikrein family – role in semen liquefaction and degradation of extracellular matrix proteins in the interstitial area surrounding Leydig cells of the adult mouse testes ( Klk1b27 , Klk1b21 , Klk1b24 ) [Michaelis et al 2017; Marques et al , 2016, Du Plessis et al , 2013; Fink et al , 2007].…”

Section: Discussionmentioning

confidence: 99%

Tcte1knockout influence on energy chain transportation, apoptosis and spermatogenesis – implications for male infertility

Olszewska

Malcher

Stokowy

et al. 2022

Preprint

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STUDY QUESTION: Is Tcte1 mutation causative for male infertility? SUMMARY ANSWER: Collected data underline the complex and devastating effect of the single-gene mutation on testicular molecular network, leading to male reproductive failure. WHAT IS KNOWN ALREADY: Latest data revealed mutations in genes related to axonemal dynein arms as causative for morphology and motility abnormalities in spermatozoa of infertile males, including dysplasia of fibrous sheath (DFS) and multiple morphological abnormalities in the sperm flagella (MMAF). The nexin-dynein regulatory complex (N-DRC) coordinates the dynein arm activity, and is built from DRC1-DRC7 proteins. DRC5 (TCTE1) - one of N-DRC element, has been already reported as a candidate for abnormal sperm flagella beating, however, only in restricted manner with no clear explanation of respective observations. STUDY DESIGN, SIZE, DURATION: Using CRISPR/Cas9 genome editing technique, mouse knockout line of Tcte1 gene was created on the basis of C57Bl/6J strain. Then, the mouse reproductive potential, semen characteristics, testicular gene expression level, sperm ATP and testis apoptosis level measurements have been performed, followed by visualization of N-DRC proteins in sperm, and protein modeling in silico. Also, a pilot genomic sequencing study of samples from human infertile males (n=248) was applied for screening of TCTE1 variants. PARTICIPANTS/MATERIALS, SETTING, METHODS: To check the reproductive potential of KO mice, adult animals were crossed for delivery of three litters per caged pair, but no longer than for 6 months, in various combinations of zygosity. All experiments were performed for wild type (WT - control group), heterozygous Tcte1+/-, and homozygous Tcte1-/- male mice. Gross anatomy was performed on testis and epididymis, followed by semen analysis. Sequencing of RNA (RNAseq; Illumina) has been done for mice testis tissues. STRING interactions have been checked for protein-protein interactions, based on changed expression level of corresponding genes identified in the mouse testis RNAseq experiments. Immunofluorescence in situ staining was performed to detect the N-DRC complex proteins: Tcte1 (Drc5), Drc7, Fbxl13 (Drc6), and Eps8l1 (Drc3) in mouse spermatozoa. To determine the ATP amount in spermatozoa, the luminescence level was measured. Also, immunofluorescent in situ staining was performed to check the level of apoptosis via caspase 3 visualization on mouse testis samples. DNA from whole blood samples of infertile males (n=137 non-obstructive azoospermia or cryptozoospermia, n=111 samples with spectrum of oligoasthenoteratozoospermia, including n=47 with asthenozoospermia) has been extracted to perform genomic sequencing (WGS, WES or Sanger). Protein prediction modeling of human identified variants and the exon 3 structure deleted in mouse knockout has been also performed. MAIN RESULTS AND THE ROLE OF CHANCE: No progeny at all was found for homozygous males with revealed oligoasthenoteratozoospermia, while heterozygous animals (fertile) manifested oligozoospermia, suggesting haploinsufficiency. RNA-sequencing of the testicular tissue showed the influence of Tcte1 mutations on the expression pattern of 21 genes responsible for mitochondrial ATP processing, linked with apoptosis, or spermatogenesis. In Tcte1-/- males the protein revealed only residual amounts in sperm head nucleus, and was not transported to sperm flagella, as other N-DRC components. Decreased ATP level (2.4-fold lower) was found in spermatozoa of homozygous mice, together with disturbed tail:midpiece ratio, leading to abnormal sperm tail beating. Casp3-positive signals (indicating apoptosis) were observed in spermatogonia only, at similar level in all three mouse genotypes. Mutation screening of human infertile males revealed 1 novel and 5 ultrarare heterogeneous variants (predicted as disease causing) in 6.05% of patients studied. Protein prediction modeling of identified variants revealed changes in the protein surface charge potential, leading to disruption in helix flexibility or its dynamics, thus, suggesting the disrupted TCTE1 interaction with its binding partners located within the axoneme.

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Recapitulation of gametic DNA methylation and its post-fertilization maintenance with reassembled DNA elements at the mouse Igf2/H19 locus

Cited by 11 publications

References 34 publications

The transgenic IG-DMR sequence of the mouse Dlk1-Dio3 domain acquired imprinted DNA methylation during the post-fertilization period

The transgenic IG-DMR sequence of the mouse Dlk1-Dio3 domain acquired imprinted DNA methylation during the post-fertilization period

Maternal DNMT3A-dependent de novo methylation of the paternal genome inhibits gene expression in the early embryo

Tcte1knockout influence on energy chain transportation, apoptosis and spermatogenesis – implications for male infertility

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