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[Dystopya]

http://www.technolog...uture-treatment


New insights into the emergence of lymphomas and colon or breast cancers - Possible future treatment


Researchers of the Ludwig-Maximilians-University in Munich found out that a vicious circle promotes the growth of tumor cells in cancer types such as lymphomas and colon or breast cancers. Normally certain machanisms ensure that pre-malignant cells are induced to enter a senescent, non-dividing state or to undergo apoptosis, i.e. commit suicide. But here the regulatory protein c-MYC and the enzyme SIRT1 form a positive feedback loop which promotes each other´s activity , subverting these control mechanisms so that cells can proliferate unchecked and facilitating the growth of tumors this way. The results could be the basis for new treatment options interrupting this feedback loop. Furthermore the findings raise questions regarding the allegedly positive effect of a daily glass of red wine on lifespan, which has been attributed in part to the activation of SIRT1 by the compound resveratrol, which is found in red wine.

Cancer cells are essentially immortal. The acquisition of an unlimited capacity to divide – the process of immortalization - is a central event in the genesis of tumors. Normally, cells are subject to stringent mechanisms which control their proliferation. Together these ensure that pre-malignant cells are induced to enter a senescent, non-dividing state or to undergo apoptosis, i.e. commit suicide. A research team led by Professor Heiko Hermeking and Dr. Antje Menssen from LMU’s Institute of Pathology has now discovered how the regulatory protein c-MYC subverts these controls, thus facilitating the growth of tumors. High levels of c-MYC, which are present in most tumor cells, activate SIRT1, an enzyme that inhibits both senescence and apoptosis. The new results show that the two proteins actually form a positive feedback loop, in that SIRT1 also promotes the activity of c-MYC. Normal cells avoid this vicious circle because they keep the gene that codes for c-MYC turned off, unless they receive growth-promoting signals. In tumor cells, this mechanism no longer functions and the cells can proliferate unchecked. Their latest findings have implications for cancer treatment, as Menssen explains: “Our results indicate that tumor types in which c-MYC plays a crucial role, such as lymphomas and colon or breast cancers, should be especially susceptible to pharmacological inhibitors that interrupt the feedback loop. In particular, combinations of drugs that interact with different components of the loop could provide a new route to effective therapies of these malignancies.” (PNAS 19.-23.12)

The c-MYC protein is involved in the control of many basic biological functions, including cell growth and division. It is therefore vital for processes that require cell proliferation, such as embryonic development and the generation of all the cell types in the blood. Overproduction of c-MYC, on the other hand, can have lethal consequences for the organism. Continuous synthesis of c-MYC is a prominent feature of immortalized cells, which divide in an uncontrolled fashion and thus facilitate the formation of tumors. Normally, multiple mechanisms serve to regulate the expression of the gene for c-MYC, and keep the level of the protein present in cells within appropriate limits. In essence, the gene is activated only when a cell is instructed to do so by specific growth-promoting signals. If this failsafe mechanism is disabled, a second internal system switches in. This back-up circuit ensures that increased concentrations of c-MYC cause premature cell senescence (which makes cells unresponsive to growth signals) and induce programmed cell death. However, in tumor cells, these safeguards no longer function – and in some tumors and cell types it has emerged that c-MYC itself is responsible for knocking them out. “How c-MYC achieves this has remained largely unclear,” says Hermeking. In order to clarify the mechanisms involved, the researchers focused on the enzyme SIRT1 as a possible accomplice of c-MYC. As Hermeking explains, “SIRT1 seemed to us a likely candidate because a related enzyme has been shown to play a role in extending the lifespan of cells in lower organisms. In human cells, SIRT1 is known to inhibit a regulator that promotes senescence and programmed cell death.”

The hunch turned out to be correct, since the team, which included molecular biologists from Aachen University and the Karolinska Institute in Stockholm, was able to show that c-MYC actually enhances SIRT1 function in a number of different ways. First, it activates NAMPT (nicotinamide phosphoribosyltransferase), which is responsible for the synthesis of a molecule required for the action of SIRT1. Secondly, c-MYC represses an inhibitor of SIRT1, so releasing a further brake on its function. Finally, SIRT1 itself potentiates these effects by reducing the rate of degradation of c-MYC. The end result is a positive feedback loop which drives the continuous accumulation of both SIRT1 and c-MYC in the cell.

The c-MYC protein is synthesized in large amounts in most tumors. Furthermore, in certain cancers, such as lymphomas and cancers of the colon and the breast, c-MYC is known to play a causative role in the origin of the primary tumor. In these cases, mutations in the c-MYC gene itself, or in genes that regulate its expression, result in constant production of the c-MYC protein. The new findings are thus of particular relevance for the development of new treatment options for these types of cancer, since one would expect them to be highly sensitive to direct inhibition of SIRT1 or NAMPT. Interestingly, several studies in recent years have revealed that levels of NAMPT are also increased in many tumors. Indeed, a chemical inhibitor of NAMPT is already undergoing clinical trials. “Our study strongly suggests that the feedback loop initiated by excess c-MYC drives the overproduction of NAMPT. A combination of drugs that would allow us to inhibit the actions of both SIRT1 and NAMPT might therefore have a synergistic effect and could open up new therapeutic possibilities,” Menssen points out.

In addition, the new findings raise questions regarding the allegedly positive effect of a daily glass of red wine on lifespan. The putative health benefits of this regime have been attributed in part to the activation of SIRT1 by the compound resveratrol, which is found in red wine. Indeed, commercial development of pharmacological SIRT1 activators such as resveratrol is already underway – in the hope that they will slow the aging process and block the development of obesity and diabetes. In this context, Hermeking advises caution: “In the light of our results, these agents should only be used after further extensive study.”

The project was supported by a Habilitation Fellowship (funded by the Exzellence Initiative at LMU) to Dr. Antje Menssen, and by the Deutsche Krebshilfe e.V. and the Max-Planck-Society. (göd)

Publication:
The c-MYC oncoprotein, the NAMPT enzyme, the SIRT1 inhibitor DBC1, and the SIRT1 deacetylase form a positive feedback loop.
A. Menssen, P. Hydbring, K. Kapelle, J. Vervoorts, J. Diebold, B. Lüscher, L.- G. Larsson, H. Hermeking
PNAS Early Edition 19.-23.12.2011
doi: 10.1073/pnas.1105304109

[maxwatt]

We have recently had posted to this group a study showing that sirt1 does not activate reseratrol but acts on a diferent pathway, another showing doses on the order of one gram is needed for resveratrol to have an effect. Two years ago a study showing putative Sirt1 activation by resveratrol was due instead to interaction with the substrate used to measure Sirt1 actiity. A year after that, a study showing that by a different assay resveratrol did indeed activate Sirt1, but that a number of other compounds, including luteolin, activated it mnore strongluy. Additionally thiee are studies showing resveratrol induces apoptosis (kills) breast cancer cells in vitro, at concentrations that might be attainable by oral administration. I know of two cases in canines where resveratrol administration appeared to reverse advanced mammary cancers.

So take the above study with a grain of salt.

[brunotto]

Conclusions: This study suggests that atorvastatin upregulates SIRT1 expression via inhibiting miR-34a in CAD patients, possibly contributing to the beneficial effects of atorvastatin on endothelial function in this

disorder.http://circ.ahajourn...bstracts/A11510

[hav]

Here's the actual abstract of the study:
http://www.ncbi.nlm....d?term=22190494

Silent information regulator 1 (SIRT1) represents an NAD(+)-dependent deacetylase that inhibits proapoptotic factors including p53. Here we determined whether SIRT1 is downstream of the prototypic c-MYC oncogene, which is activated in the majority of tumors. Elevated expression of c-MYC in human colorectal cancer correlated with increased SIRT1 protein levels. Activation of a conditional c-MYC allele induced increased levels of SIRT1 protein, NAD(+), and nicotinamide-phosphoribosyltransferase (NAMPT) mRNA in several cell types. This increase in SIRT1 required the induction of the NAMPT gene by c-MYC. NAMPT is the rate-limiting enzyme of the NAD(+) salvage pathway and enhances SIRT1 activity by increasing the amount of NAD(+). c-MYC also contributed to SIRT1 activation by sequestering the SIRT1 inhibitor deleted in breast cancer 1 (DBC1) from the SIRT1 protein. In primary human fibroblasts previously immortalized by introduction of c-MYC, down-regulation of SIRT1 induced senescence and apoptosis. In various cell lines inactivation of SIRT1 by RNA interference, chemical inhibitors, or ectopic DBC1 enhanced c-MYC-induced apoptosis. Furthermore, SIRT1 directly bound to and deacetylated c-MYC. Enforced SIRT1 expression increased and depletion/inhibition of SIRT1 reduced c-MYC stability. Depletion/inhibition of SIRT1 correlated with reduced lysine 63-linked polyubiquitination of c-Myc, which presumably destabilizes c-MYC by supporting degradative lysine 48-linked polyubiquitination. Moreover, SIRT1 enhanced the transcriptional activity of c-MYC. Taken together, these results show that c-MYC activates SIRT1, which in turn promotes c-MYC function. Furthermore, SIRT1 suppressed cellular senescence in cells with deregulated c-MYC expression and also inhibited c-MYC-induced apoptosis. Constitutive activation of this positive feedback loop may contribute to the development and maintenance of tumors in the context of deregulated c-MYC.

The study may only pertain to the particular genetic hack of c-MYC that they employed..

Howard

[brunotto]

Maybe we have to order Niacinamide... better aging a little quicker and not have cancer...

The fact that SIRT1 is inhibited by such low concentrations of nicotinamide in vitro raises the possibility that this mode of inhibition may be physiologically relevant.

http://www.jbc.org/c...7/47/45099.full

Edited by brunotto, 01 March 2012 - 02:08 PM.

[brunotto]

Type 3 deacetylases may be the most important and they can be inhibited by the supplement niacinamide (nicotinamide). This product is NOT niacin.
Niacinamide is critically involved in inhibiting cancer cell growth and survival. This is the story.

SIRT1
SIRT1 is a so-called longevity factor which inhibits the death of cells, including cancer cells. This deacetylase shuttles back and forth between the cytoplasm and the nucleus. In the cytoplasm, it deacetylates and inhibits various anti-growth transcription factors such as p53, FOXO and PPARgamma.
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In cancer, many anti-growth genes are inactivated by the methylation of their DNA (folic acid is a methylating agent). A massive scientific literature has been published on this topic. This is step one. In step two, the methylated DNA appears to interact with histone deacetylase proteins (like sirt1). These proteins remove acetyl groups from histones, thereby inactivating their activity. Histones are necessary for the activation of specific genes. Many histone deacetylase inhibitors have been developed and are in clinical trials. The objective of these drugs is to reactivate silent genes by blocking the activity of histone deacetylase enzymes.
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This study shows that gene methylation, per se, is NOT enough to silence genes. The hypermethylated DNA apparently attracts the class 3 histone deacetylase SIRT1 to the gene and this interaction is critically important in gene silencing. If SIRT1 activity is silenced, methylated DNA does NOT silence (anthi-growth) genes. This is a remarkable observation. The activity of type 1 and 2 histone deacetylase enzymes is now irrelevant. They cannot contribute to the silencing of genes if SIRT1 is not bound to the methylated DNA.

In the nucleus, SIRT1 promotes DNA repair by the deacetylation of a major repair enzyme. If we are trying to kill cancer cells, we do not want their DNA repaired
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Nicotinamide (niacinamide) is the NATURAL inhibitor of SIRT1 activity. As such, it is a powerful anti-cancer compound and a type 3 histone deacetylase inhibitor.
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http://www.infoisus....ntiinflamm.html

Edited by brunotto, 01 March 2012 - 05:00 PM.

[maxwatt]

If you want to inhibit sirt1 myricetin or quercetin might also be effective. Niacinamide actually activates SIRT1, and only inhibits it at higher concentrations, so you may be activating Sirt1 most of the time if you supplement with it. But it is more complex than that. Niacinamide increases NAD levels, increasing the NAD/NADH ratio, as does caloric restriction, and is thought to be a mechanism if CR's life extending effect.

It is odd how we get papers claiming resveratrol does not activate sirt1, or that it has a different mechanism of action, and now we have one claiming resveratrl is dangerous because it activates SIRT1, and sirt1 induces cancer. I think this is over-interpretation of what is a dubious study to begin with. Resveratrol has been shown inmany studies to induce apoptosis (cell death) in cancer cells, which is the opposite of what one would expect if the conclusions of the study cited by the OP at the start of this thread were valid.

Below are some papers showing resveratrol kills cancer cells.

Resveratrol Inhibits Proliferation and Induces Apoptosis through the Hedgehog Signaling Pathway in Pancreatic Cancer Cell.
Mo W, Xu X, Xu L, Wang F, Ke A, Wang X, Guo C.
Pancreatology. 2012;11(6):601-9. Epub 2012 Feb 2.

PMID: 22301921

Anticancer Agents Med Chem. 2012 Jan 31. [Epub ahead of print]
Regulation of Cell Death And Survival By Resveratrol: Implications For CancerTherapy.

Fulda S.

Institute for Experimental Cancer Research in Pediatrics, Goethe-University Frankfurt, Komturstr. 3a, 60528 Frankfurt, Germany. simone.fulda@kgu.de.

Abstract
Tissue homeostasis is maintained by tight control of signaling events that regulate cell death and cell survival. In addition, the antitumor activity of most cancer therapies, including chemotherapy, radiotherapy or immunotherapy, is mediated by the activation of apoptosis in cancer cells. Apoptosis (programmed cell death) is a key regulatory mechanism that is critical to monitor tissue homeostasis during development as well as various organs of the adult organism. Accordingly, too little apoptosis can contribute to the pathogenesis of many human diseases, including cancer. Natural compounds, e.g. polyphenols such as resveratrol, have emerged as promising agents for cancer chemoprevention and therapy, since they interfere with various major signaling cascades that are aberrantly regulated in cancers. For example, resveratrol can antagonize signal transduction pathways that prevent apoptosis or support cancer cell proliferation. Further elucation of the molecular signaling events that are regulated by resveratrol is anticipated to path the way for the transfer of resveratrol and its derivatives into clinical application for chemoprevention or treatment of human cancer.
PMID 22292764

Resveratrol induces apoptosis via ROS-triggered autophagy in human colon cancer cells.

Miki H, Uehara N, Kimura A, Sasaki T, Yuri T, Yoshizawa K, Tsubura A.
Int J Oncol. 2012 Apr;40(4):1020-8. doi: 10.3892/ijo.2012.1325. Epub 2012 Jan 3.

PMID: 22218562

Edited by maxwatt, 03 March 2012 - 06:53 PM.