Registration for a live webinar on 'Precision medicine treatment for anticancer drug resistance' is now open.
See webinar detailsWe noted you are experiencing viewing problems
-
Check with your IT department that JWPlatform, JWPlayer and Amazon AWS & CloudFront are not being blocked by your network. The relevant domains are *.jwplatform.com, *.jwpsrv.com, *.jwpcdn.com, jwpltx.com, jwpsrv.a.ssl.fastly.net, *.amazonaws.com and *.cloudfront.net. The relevant ports are 80 and 443.
-
Check the following talk links to see which ones work correctly:
Auto Mode
HTTP Progressive Download Send us your results from the above test links at access@hstalks.com and we will contact you with further advice on troubleshooting your viewing problems. -
No luck yet? More tips for troubleshooting viewing issues
-
Contact HST Support access@hstalks.com
-
Please review our troubleshooting guide for tips and advice on resolving your viewing problems.
-
For additional help, please don't hesitate to contact HST support access@hstalks.com
We hope you have enjoyed this limited-length demo
This is a limited length demo talk; you may
login or
review methods of
obtaining more access.
Printable Handouts
Navigable Slide Index
- Epigenetic control by histone methylation
- Info stored in DNA sequence-question
- Power of genetic control
- Diversity of stored information in DNA template
- Mechanisms to induce heterochromatic structures
- Discovery of first HMTase
- SUV39H-HP1 methylation system
- Histone lysine methylation systems
- Specificity of H3-K9 methylation antibodies
- Histone lysine methylation patterns
- Summary of analysis with selective anti-bodies
- Suv39h/Suv4-20h - different substrate specificities
- Constitutive heterochromatin
- Complexity of distinct histone-lysine marks
- Activating modifications
- Reversibility of histone methylation
- Repressing modifications
- Reprograming through oocyte cytoplasm
- Experiments relating to an early embryogenisis
- Cancer and Epigenetics
- Reactivation of tumor suppressor genes
- Global histone modification patterns
- Epigenomes
- Chromosome landscaping
- Repeat sequences in mouse genome
- ChIP on chip micro array
- H3-K9 tri-methylation
- RNA generated from repetitive elements
- Primary triggers to discriminate chromatins
- Chromosomes under distinct epigenetic states
- Big questions in epigenetic research
- The epigenome network
- NOE members
- Acknowledgements
- Thanks to colleagues in the laboratory
Topics Covered
- The diversity of covalent histone tail modifications for imparting epigenetic information
- observations of robust histone modifications at silent chromatin regions
- the representation of repressive histone marks as indications of epigenetic plasticity in different cells
- analysis of the profiles of normal and aberrant histone lysine methylation patterns, as they occur during the transition of an embryonic to a differentiated cell or in controlled self-renewal vs. pro-neoplastic or metastatic conditions
- elucidation of these histone modification patterns for novel advances in stem cell research, nuclear reprogramming and cancer
Talk Citation
Jenuwein, T. (2022, April 12). Epigenetic control by histone methylation [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved December 27, 2024, from https://doi.org/10.69645/ZUVF1330.Export Citation (RIS)
Publication History
Financial Disclosures
- Prof. Thomas Jenuwein has not informed HSTalks of any commercial/financial relationship that it is appropriate to disclose.
Epigenetic control by histone methylation
A selection of talks on Cell Biology
Transcript
Please wait while the transcript is being prepared...
0:00
Henry Stewart Lectures Epigenetics 2005.
Epigenetic Control by Histone Methylation.
Thomas Jenuwein, Senior Scientist, IMP Vienna.
0:12
I would like to start my lecture by illustrating the problem that I will be discussing,
which is the question whether the information that is stored in
the DNA sequence will be sufficient to allow multicellular development to proceed,
or whether there are additional mechanisms that help to
facilitate and potentiate genetic information.
We now know the DNA sequence of many modern organisms ranging from unicellular organisms,
such as yeasts to the human genome,
and there are around 35,000 genes in
the human genome giving rise to more than 200 cell types.
However, we are still far from understanding what is
the molecular makeup of a stem cell based on a fully differentiated cell,
or how does a young cell differ from an aged cell.
And is all the information that is required to differentiate
these cell types only residing in the DNA sequence
or are there other mechanisms that help to stabilize it?
1:13
Now, I would like to highlight this distinction,
by first discussing what the power of genetic control can do,
and this is shown on the left hand side.
Now genetic control involves mutations of the DNA sequence.
These are alterations that are introduced,
and indicated here by the red asterisks.
As such, mutations of the DNA sequence can be stably inherited.
They will be propagated through the germ line,
and if they accumulate and prevent the pairing of homologous chromosomes,
they will also prevent the propagation of the genetic information,
and can define a novel species barriers.
In contrast to genetic control,
epigenetic control does not alter the DNA sequence.
But epigenetic control, rather,
is mediated towards the chromatin template.
The DNA polymer is not presented as a naked molecule in living cells,
but the physiological template is chromatin,
and that is shown by the four nucleosomes around which the DNA polymer is wrapped.
Each nucleosome consists of histone molecules.
These histone molecules have flexible amino-termini,
shown here in black.
They are a variety of epigenetic modifications or
alterations that can impinge on the chromatin structure,
and they range from modifications of the histone termini.
They also include DNA methylation,
shown here by the red hexagon.
They also involve exchange of histone variants,
indicated by the light colored nucleosome,
and many other mechanisms that I will discuss in the course of this lecture.
One of the big questions in epigenetic research is how
stable are these alterations on the chromatin template?
Will they only be propagated in somatic cells,
or can we also identify imprints in the germ line?
And what is it really,
how can they contribute to the variability of this thing,
cellular phenotypes, during multicellular development?
The question of diversity and how the genetic information that is stored in