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Growths in Your Colon Aren’t Fun, Get Yourself Some LKB1! Abstract Billions of dollars are being poured into the research of cancer, the National Cancer Institute alone spends $4.9 Billion every year. Liver Kinase B1 (LKB1) stands out as one important protein that regulates cell metabolism, cell division, and therefore, cancerous growth. LKB1 is a key regulator of cell metabolism and cell division by acting as a tumor suppressor by turning on other proteins that suppress tumor growth. Human mutations in LKB1 causes the disease Peutz-Jeghers syndrome, which results in benign tumor-like growth called polyps in the intestine and a 50% chance of developing cancer by the age of 50. When cell energy, ATP, is low LKB1 will be activated. Active LKB1 regulates the activity of adenosine monophosphate-activated protein kinase (AMPK). LKB1 directly activates AMPK by adding a phosphate group to Thr-172. AMPK activity increases the production of ATP by activating glycolysis and fatty acid oxidation. AMPK can also decrease the amount of energy needed by the cell by inhibiting protein synthesis and cell growth. Both of these processes play a role in cancer development. Drugs like Metformin, a successful diabetic drug, are thought to activate LKB1. Through the activation of AMPK to cease cancerous growth, and with the whole cascade of proteins ceases cancerous growth. LKB1 Mutations and Consequences Peutz-Jeghers syndrome is characterized by polyps that form inside the intestine (Calva et al 2008). An example of intestinal polyps in mice is shown in figure # 5. Patients with Peutz-Jeghers syndrome are prone to colon and rectal cancers as well as a wide variety of other cancers (Boardman et al., 1998). All cancers, such as those listed, develop when cells rapidly divide in an area, and grow out of control. This growth is called a tumor, and it can result in serious health issues health issues. The process of rapid cell division requires a lot of cellular energy in the form of ATP. When energy levels decrease, the cell activates a stress response protein called Liver kinase B1 (LKB1) that will cause the cell to slow down the energy consuming processes such as cell proliferation and protein production and will turn on energy producing processes such as metabolism. by phosphorylating and activating 5' adenosine monophosphate-activated protein kinase (AMPK) (Reference). When LKB1 is mutated or missing such as in Peutz-Jeghers syndrome, the cancer cells have defective energy stress response and continue to proliferate uncontrollably (Reference). LKB1 in Mouse Embryos LKB1 is expressed in all cell types and appears to be important for early mouse development. When LKB1 is knockout or deleted (-/-) there are serious defects in blood vessels as shown in Figure 2 (reference). A is an image of an early mouse embryo (embryonic day 8.5) that shows the development of the aorta in both a LKB1 knockout mouse (-/-) and a wildtype mouse, (+/+). The mutated aorta of the knockout mouse is smaller in diameter. B is an image of a slightly older embryo (embryonic day 9.5), and the arrow points to where the aorta is discontinuous in the knockout mouse (right), and the corresponding area in the wildtype mouse, (+/+). C is an image of an embryonic day 9.5 head and shows the tissue of the embryo that will develop into the brain. In the knockout mouse, (-/-), the mesenchyme layer is not fully developed, as displayed by the asterisks. Metformin Activating ATM ~~~~~this far in editing~~~~~ Metformin activates Ataxia Telangiectasia Mutated (ATM) which is a serine/threonine protein kinase responsible for the phosphorlation Liver Kinase B1 (LKB1) It is supposed to be activated by DNA double-strand breaks however sometimes they do not function accordingly The activation of ATM and the phosphorlation of LKB1 guides the LKB1 out of the nucleus and into the cytosol Adenosine-monophosphate Activated Kinase (AMPK) is abundant in the cytosol and that is where LKB1 is able to phosphorlate AMPK and continue the cycle Phosphorylated LKB1 Above is an image of two cells, both with LKB1 mutation resulting in the lack of Adenosine-monophosphate Activated Kinase (AMPK) phosphorylation. The one with Metformin results in more LKB1 and AMPK interaction and thus AMPK phosphorylation versus the control. Metformin, a popular anti diabetic drug, activates AMPK by extracting Live Kinase B1 out from the nucleus and into the cytoplasm where AMPK is generally locates. It does this by phosphorylating LKB1 at Ser428 which then helps LKB1 export from the nucleus and meet with AMPK in the cytoplasm, hence phosphorylating AMPK and continuing the natural cycle. Liver Kinase B1 has vital functions inside the cell. It is clear that the proper activation of LKB1 results in the control over the proliferation, cellular metabolism, and cellular integrity of the cell. As a kinase its sole purpose is to phosphorlate making it a stepping stone inside of an important cellular cycle. This cellular cycle is a broad cycle which acts as a check point for the cell. Without this checkpoint the cell would be left helpless in managing its most important components. This would ultimately disrupt the overall homeostasis of the cell and most importantly, if not targeted by apoptosis, have the ability to turn cancerous. Functions of LKB1 LKB1 works as a complex of three parts: LKB1, the pseudokinase STRAD, and MO25 (reference). When LKB1 is activated, it in turn activates AMPK by phosphorylating the Threonine 172 amino acid residue (reference). AMPK also is activated by low blood oxygen, as well as low blood glucose (reference). Once activated, AMPK can turn on catabolic pathways that produce ATP such. Glucose metabolism defects in glucose metabolism and inhibit anabolic pathways such as cell growth and protein synthesis. Since defects in glucose metabolism can result in diabetes, it is not surprising that LKB1 dysfunction has been linked to diabetes (reference). There are drugs like Metformin that activate LKB1 indirectly in order to treat those with diabetes. LKB1 and AMPK are also involved in regulating cell polarity and cell growth (reference). If either of these processes is not functioning properly, uncontrolled cell growth (cancer) can occur. SMART Teams are supported by the National Center for Advancing Translational Sciences, National Institutes of Health, through Grant Number 8UL1TR000055. Its contents are solely the responsibility of the authors and do not necessarily represent the official views of the NIH. Citations Shaw, R. (2011). The cancer connection. Drugs, diabetes and cancer, 470(338). Xie, Z., Dong, Y., Scholtz, R., Neumann, D., & Zou, M. (2008). Phosporylation of lkb1 at serine 428 by protein kinase c is required for metformin-enchanced activation of the amp-activated protein kinase in endothelial cells. Circulation,117, 952-962. Ylikorkala, A., Rossi, D. J., Korsisaali, N., Luukko, K., Alitalo, K., Henkemeyer, M., & Makela, T. P. (2001). Vascular abnormalities and deregulation of vegf in lkb1-deficient mice. Sciencemag, 293, 1323-1326. Zhao, R., & Xu, Z. (2014). The biological functions of lkb1.Targeting the LKB1 Tumor supressor, 32-52. Acknowledgements We would like to thank Dr. Stephanie Cossette for continuing to help and support us through the process of learning and presenting information about molecular biology. Not only do we now know the specific information, but because of her efforts, we got a glimpse of the work researchers do daily, and the work that goes into it.
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