Dual Roles for Nuclear RNAi Argonautes in C. elegans Dosage Compensation

Dosage compensation involves chromosome-wide gene regulatory mechanisms which impact higher order chromatin structure and are crucial for organismal health. Using a genetic approach, we identified Argonaute genes which promote dosage compensation in C. elegans. Dosage compensation in C. elegans hermaphrodites is initiated by the silencing of xol-1 and subsequent activation of the Dosage Compensation Complex (DCC) which binds to both hermaphrodite X chromosomes and reduces transcriptional output by twofold. A hallmark phenotype of dosage compensation mutants is decondensation of the X chromosomes. We characterized this phenotype in Argonaute mutants using X chromosome paint probe and fluorescence microscopy. We found that while nuclear Argonaute mutants hrde-1 and nrde-3 exhibit de-repression of xol-1 transcripts, they also effect X chromosome condensation in a xol-1-independent manner. We also characterized the physiological contribution of Argonaute genes to dosage compensation using genetic assays and find that hrde-1 and nrde-3, together with the piRNA Argonaute prg-1, contribute to healthy dosage compensation both upstream and downstream of xol-1.

Download Full-text

SDC-3 coordinates the assembly of a dosage compensation complex on the nematode X chromosome

Development ◽

10.1242/dev.124.5.1019 ◽

1997 ◽

Vol 124 (5) ◽

pp. 1019-1031 ◽

Cited By ~ 1

Author(s):

T.L. Davis ◽

B.J. Meyer

Keyword(s):

Zinc Finger ◽

X Chromosome ◽

Dosage Compensation ◽

Protein Complex ◽

Terminal Region ◽

X Chromosomes ◽

C Elegans ◽

Amino Terminal ◽

Zinc Finger Motifs ◽

Specific Association

X chromosome expression in C. elegans is controlled by a chromosome-wide regulatory process called dosage compensation that specifically reduces by half the level of transcripts made from each hermaphrodite X chromosome. This process equalizes X expression between the sexes (XX hermaphrodites and XO males), despite their two-fold difference in X chromosome dose, and thereby prevents sex-specific lethality. Dosage compensation is achieved by a protein complex that associates with X in a sex-specific fashion to modulate gene expression. SDC-3, a protein that coordinately controls both sex determination and dosage compensation, activates dosage compensation by directing the dosage compensation protein complex to the hermaphrodite X chromosomes. We show that SDC-3 coordinates this assembly through its own sex-specific association with X. SDC-3 in turn requires other members of the dosage compensation gene hierarchy for its stability and its X localization. In addition, SDC-3 requires its own zinc finger motifs and an amino-terminal region for its X association. Our experiments suggest the possible involvement of zinc finger motifs in X chromosome recognition and the amino-terminal region in interactions with other dosage compensation proteins.

Download Full-text

The H4K20 demethylase DPY-21 regulates the dynamics of condensin DC binding

Journal of Cell Science ◽

10.1242/jcs.258818 ◽

2021 ◽

Author(s):

Laura Breimann ◽

Ana Karina Morao ◽

Jun Kim ◽

David Sebastian Jimenez ◽

Nina Maryn ◽

...

Keyword(s):

X Chromosome ◽

Dosage Compensation ◽

Transcriptional Repression ◽

Fluorescence Recovery After Photobleaching ◽

Null Mutant ◽

Wild Type ◽

X Chromosomes ◽

C Elegans ◽

Catalytic Role ◽

Mobile Fraction

Condensin is a multi-subunit SMC complex that binds to and compacts chromosomes. Here we addressed the regulation of condensin binding dynamics using C. elegans condensin DC, which represses X chromosomes in hermaphrodites for dosage compensation. We established fluorescence recovery after photobleaching (FRAP) using the SMC4 homolog DPY-27 and showed that a well-characterized ATPase mutation abolishes its binding. Next, we performed FRAP in the background of several chromatin modifier mutants that cause varying degrees of X-chromosome derepression. The greatest effect was in a null mutant of the H4K20me2 demethylase DPY-21, where the mobile fraction of condensin DC reduced from ∼30% to 10%. In contrast, a catalytic mutant of dpy-21 did not regulate condensin DC mobility. Hi-C data in the dpy-21 null mutant showed little change compared to wild type, uncoupling Hi-C measured long-range DNA contacts from transcriptional repression of the X chromosomes. Together, our results indicate that DPY-21 has a non-catalytic role in regulating the dynamics of condensin DC binding, which is important for transcription repression.

Download Full-text

Absence of X-chromosome dosage compensation in the primordial germ cells of Drosophila embryos

Scientific Reports ◽

10.1038/s41598-021-84402-7 ◽

2021 ◽

Vol 11 (1) ◽

Author(s):

Ryoma Ota ◽

Makoto Hayashi ◽

Shumpei Morita ◽

Hiroki Miura ◽

Satoru Kobayashi

Keyword(s):

X Chromosome ◽

Germ Cells ◽

Dosage Compensation ◽

Sex Chromosome ◽

Primordial Germ Cells ◽

Histone H4 ◽

X Chromosomes ◽

Essential Components ◽

Msl Complex ◽

Male Specific

AbstractDosage compensation is a mechanism that equalizes sex chromosome gene expression between the sexes. In Drosophila, individuals with two X chromosomes (XX) become female, whereas males have one X chromosome (XY). In males, dosage compensation of the X chromosome in the soma is achieved by five proteins and two non-coding RNAs, which assemble into the male-specific lethal (MSL) complex to upregulate X-linked genes twofold. By contrast, it remains unclear whether dosage compensation occurs in the germline. To address this issue, we performed transcriptome analysis of male and female primordial germ cells (PGCs). We found that the expression levels of X-linked genes were approximately twofold higher in female PGCs than in male PGCs. Acetylation of lysine residue 16 on histone H4 (H4K16ac), which is catalyzed by the MSL complex, was undetectable in these cells. In male PGCs, hyperactivation of X-linked genes and H4K16ac were induced by overexpression of the essential components of the MSL complex, which were expressed at very low levels in PGCs. Together, these findings indicate that failure of MSL complex formation results in the absence of X-chromosome dosage compensation in male PGCs.

Download Full-text

Parallel Universes for Models of X Chromosome Dosage Compensation in Drosophila: A Review

Cytogenetic and Genome Research ◽

10.1159/000445924 ◽

2016 ◽

Vol 148 (1) ◽

pp. 52-67 ◽

Cited By ~ 11

Author(s):

James A. Birchler

Keyword(s):

X Chromosome ◽

Dosage Compensation ◽

Sex Chromosome ◽

Fold Increase ◽

Molecular Data ◽

X Chromosomes ◽

Histone Modifiers ◽

Parallel Universes ◽

Msl Complex ◽

High Level

Dosage compensation in Drosophila involves an approximately 2-fold increase in expression of the single X chromosome in males compared to the per gene expression in females with 2 X chromosomes. Two models have been considered for an explanation. One proposes that the male-specific lethal (MSL) complex that is associated with the male X chromosome brings histone modifiers to the sex chromosome to increase its expression. The other proposes that the inverse effect which results from genomic imbalance would tend to upregulate the genome approximately 2-fold, but the MSL complex sequesters histone modifiers from the autosomes to the X to mute this autosomal male-biased expression. On the X, the MSL complex must override the high level of resulting histone modifications to prevent overcompensation of the X chromosome. Each model is evaluated in terms of fitting classical genetic and recent molecular data. Potential paths toward resolving the models are suggested.

Download Full-text

Developmental Dynamics of X-Chromosome Dosage Compensation by the DCC and H4K20me1 in C. elegans

PLoS Genetics ◽

10.1371/journal.pgen.1005698 ◽

2015 ◽

Vol 11 (12) ◽

pp. e1005698 ◽

Cited By ~ 24

Author(s):

Maxwell Kramer ◽

Anna-Lena Kranz ◽

Amanda Su ◽

Lara H. Winterkorn ◽

Sarah Elizabeth Albritton ◽

...

Keyword(s):

X Chromosome ◽

Dosage Compensation ◽

C Elegans ◽

Developmental Dynamics

Download Full-text

The C. elegans Dosage Compensation Complex Propagates Dynamically and Independently of X Chromosome Sequence

Current Biology ◽

10.1016/j.cub.2009.09.047 ◽

2009 ◽

Vol 19 (21) ◽

pp. 1777-1787 ◽

Cited By ~ 25

Author(s):

Sevinç Ercan ◽

Lindsay L. Dick ◽

Jason D. Lieb

Keyword(s):

X Chromosome ◽

Dosage Compensation ◽

Dosage Compensation Complex ◽

C Elegans ◽

Chromosome Sequence

Download Full-text

Gene action in the mammalian X-chromosome

Genetics Research ◽

10.1017/s0016672300010624 ◽

1967 ◽

Vol 9 (3) ◽

pp. 343-357 ◽

Cited By ~ 13

Author(s):

Hans Grüneberg

Keyword(s):

X Chromosome ◽

Dosage Compensation ◽

Gene Action ◽

X Chromosomes ◽

Independent Evidence ◽

Partial Inhibition ◽

Lyon Hypothesis ◽

New Hypothesis

Contrary to opinions expressed by various authors, the phenotype of heterozygotes for mammalian sex-linked genes gives no support for the Lyon hypothesis (L.H.). Evidence, mainly from the mouse, shows that in such heterozygotes, both alleles act together as in autosomal genes.In the present paper, it is shown that neither the behaviour of double heterozygotes for sex-linked genes nor that of X-autosome translocations provides independent evidence in favour of the L.H.: in each case, the interpretation depends on that of the behaviour of single heterozygotes and hence fails to discriminate. Moreover, new facts from both types of situation are also contrary to the L.H. In particular, a unified interpretation which fits the behaviour of genes in all known types of X-autosome translocations in the mouse requires the assumption that partial inhibition of gene action happens in both X-chromosomes of mouse females, and presumably the females of other mammals. The new hypothesis is consistent with all relevant genetical facts and, like the L.H., it also accounts for dosage compensation.

Download Full-text

GA-repeats on mammalian X chromosomes support Ohno’s hypothesis of dosage compensation by transcriptional upregulation

10.1101/485300 ◽

2018 ◽

Author(s):

Edridge D’Souza ◽

Elizaveta Hosage ◽

Kathryn Weinand ◽

Steve Gisselbrecht ◽

Vicky Markstein ◽

...

Keyword(s):

Gene Expression ◽

Transposable Elements ◽

X Chromosome ◽

Dosage Compensation ◽

Binding Sites ◽

Convergent Evolution ◽

Fruit Fly ◽

Dosage Compensation Complex ◽

X Chromosomes ◽

Repeat Sequences

ABSTRACTOver 50 years ago, Susumo Ohno proposed that dosage compensation in mammals would require upregulation of gene expression on the single active X chromosome, a mechanism which to date is best understood in the fruit fly Drosophila melanogaster. Here, we report that the GA-repeat sequences that recruit the conserved MSL dosage compensation complex to the Drosophila X chromosome are also enriched across mammalian X chromosomes, providing genomic support for the Ohno hypothesis. We show that mammalian GA-repeats derive in part from transposable elements, suggesting a mechanism whereby unrelated X chromosomes from dipterans to mammals accumulate binding sites for the MSL dosage compensation complex through convergent evolution, driven by their propensity to accumulate transposable elements.

Download Full-text

Dosage compensation in sciarids is achieved by hypertranscription of the single X chromosome in males.

Genetics ◽

10.1093/genetics/138.3.787 ◽

1994 ◽

Vol 138 (3) ◽

pp. 787-790

Author(s):

P R da Cunha ◽

B Granadino ◽

A L Perondini ◽

L Sánchez

Keyword(s):

X Chromosome ◽

Dosage Compensation ◽

Sex Chromosomes ◽

Sex Chromosome ◽

X Chromosomes ◽

Different Doses

Abstract Dosage compensation refers to the process whereby females and males with different doses of sex chromosomes have similar amounts of products from sex chromosome-linked genes. We analyzed the process of dosage compensation in Sciara ocellaris, Diptera of the suborder Nematocera. By autoradiography and measurements of X-linked rRNA in females (XX) and males (XO), we found that the rate of transcription of the single X chromosome in males is similar to that of the two X chromosomes in females. This, together with the bloated appearance of the X chromosome in males, support the idea that in sciarids dosage compensation is accomplished by hypertranscription of the X chromosome in males.

Download Full-text

Topoisomerases I and II facilitate condensin DC translocation to organize and repress X chromosomes in C. elegans

10.1101/2021.11.30.470639 ◽

2021 ◽

Author(s):

Ana Karina Morao ◽

Jun Kim ◽

Daniel Obaji ◽

Siyu Sun ◽

Sevinc Ercan

Keyword(s):

Long Range ◽

X Chromosome ◽

Molecular Motors ◽

Topoisomerase Ii ◽

Dna Looping ◽

Loop Formation ◽

X Chromosomes ◽

C Elegans ◽

And Control

Condensin complexes are evolutionarily conserved molecular motors that translocate along DNA and form loops. While condensin-mediated DNA looping is thought to direct the chain-passing activity of topoisomerase II to separate sister chromatids, it is not known if topological constraints in turn regulate loop formation in vivo. Here we applied auxin inducible degradation of topoisomerases I and II to determine how DNA topology affects the translocation of an X chromosome specific condensin that represses transcription for dosage compensation in C. elegans (condensin DC). We found that both topoisomerases colocalize with condensin DC and control its movement at different genomic scales. TOP-2 depletion hindered condensin DC translocation over long distances, resulting in accumulation around its X-specific recruitment sites and shorter Hi-C interactions. In contrast, TOP-1 depletion did not affect long-range spreading but resulted in accumulation of condensin DC within expressed gene bodies. Both TOP-1 and TOP-2 depletions resulted in X chromosome transcriptional upregulation indicating that condensin DC translocation at both scales is required for its function in gene repression. Together the distinct effects of TOP-1 and TOP-2 on condensin DC distribution revealed two distinct modes of condensin DC association with chromatin: long-range translocation that requires decatenation/unknotting of DNA and short-range translocation across genes that requires resolution of transcription-induced supercoiling.

Download Full-text