Mobility between different physical environments in the cell nucleus regulates the daily oscillations in the activity of genes that are controlled by the internal biological clock, according to a study that is published in the journal  Molecular Cell.  Eventually, these findings may lead to novel therapeutic strategies for the treatment of diseases linked with disrupted circadian rhythm.

So called clock-controlled, or circadian, genes are part of the internal biological clock, allowing humans and other light-sensitive organisms to adjust their daily activity to the cycle of daylight and darkness. In the current study, investigators at Sweden’s Karolinska Institutet found that daily changes in the spatial localisation of clock-controlled genes in the cell nucleus regulates fluctuations in their activity with a 24-hour period length.

“We have uncovered a novel principle of circadian transcriptional regulation that involves a so-far unexpected dynamics in the sub-nuclear positioning of circadian genes”, says principal investigator Anita Göndör at the department of microbiology, tumor and cell biology at Karolinska Institutet.

The genetic material is packaged in a structure called chromatin in the cell nucleus. It has been established that the 3-dimensional distribution of chromatin in the nucleus follows a pattern. Open chromatin containing active genes tends to occupy the central parts, whereas chromatin containing genes that are not active tends to localise to the peripheral parts of the nucleus – an environment rich in factors that promote gene silencing.

Researchers investigated physical meetings between regions that are located far apart from each other on the linear chromatin fibre or reside on different chromosomes. By studying such encounters in the 3-dimensional space of the nucleus, they discovered a network of contacts between clock-controlled genes and domains of gene-poor, repressed chromatin in the periphery of the nucleus. They identified two proteins that bring the genes to bed and help them go to sleep at the periphery of the cell nucleus every day: poly(ADP-ribose) polymerase 1 (PARP1), a well-known regulator of DNA repair and gene expression, and the transcription factor CTCF. The researchers thus found that PARP1 and CTCF promote the diurnal recruitment of circadian genes to the nuclear periphery to attenuate their expression. They were then released from the periphery in a silent, ‘sleeping’ state to start a new cycle.

The internal biological clock regulates, among other things, body temperature, metabolism and the levels of several hormones. Disruption of circadian rhythm has been linked to predisposition to multifactorial diseases, such as diabetes mellitus, metabolic syndrome, psychiatric disorders and cancer. The new knowledge may lead up to new strategies for treatment of diseases that are affected by deregulated circadian rhythm.

The research was supported by the Swedish Research Council, the Swedish Pediatric Cancer Foundation, the Swedish Cancer Foundation, the Lundberg Foundation, Karolinska Institutet, and the KA Wallenberg Foundation. Researchers from SciLifeLab in Sweden, and University of Pécs, Hungary, also contributed to this recent study.

Publication: ‘PARP1- and CTCF-Mediated Interactions between Active and Repressed Chromatin  at the Lamina Promote Oscillating Transcription’, Honglei Zhao, Emmanouil G. Sifakis, Noriyuki Sumida, Lluís Millán-Ariño, Barbara A. Scholz, J. Peter Svensson, Xingqi Chen, Anna L. Ronnegren, Carolina Diettrich Mallet de Lima, Farzaneh Shahin Varnoosfaderani, Chengxi Shi, Olga Loseva, Samer Yammine, Maria Israelsson, Li-Sophie Rathje, Balázs Németi, Erik Fredlund, Thomas Helleday, Márta P. Imreh, and Anita Göndör, Molecular Cell , publishing in the 17 September, 2015 paper issue, online 27 August 2015.

Photo: Fredrik Persson

Source: Karolinska Institutet