Lipid Kinase – Function, Significance & Medicine
Lipid kinases are enzymes that chemically modify lipids through phosphorylation, thereby controlling key signaling pathways inside cells. They play a central role in metabolism, cell growth, and immune function.
Things worth knowing about "Lipid kinase"
Lipid kinases are enzymes that chemically modify lipids through phosphorylation, thereby controlling key signaling pathways inside cells. They play a central role in metabolism, cell growth, and immune function.
What Is a Lipid Kinase?
A lipid kinase is an enzyme that transfers phosphate groups onto lipid molecules – a process called phosphorylation. Lipids are fat-like molecules that not only serve as energy carriers but also act as signaling messengers in cellular communication. Through the activity of lipid kinases, phosphorylated lipids such as phosphoinositides are generated, which function as intracellular signaling molecules that regulate a wide range of biological processes.
Biological Importance
Lipid kinases are among the most important regulators of cellular processes. They control, among other things:
- Cell growth and division: Lipid kinases such as phosphoinositide 3-kinases (PI3K) activate signaling pathways that promote cell growth and survival.
- Cell migration: The movement and migration of cells are guided by lipid-based signals.
- Immune response: Immune cells rely on lipid kinase signaling pathways to respond to infections and inflammation.
- Metabolism: Lipid kinases are involved in regulating glucose and fat metabolism.
- Membrane dynamics: They influence the transport of substances within and between cells.
Key Classes of Lipid Kinases
Phosphoinositide 3-Kinases (PI3K)
The PI3K family is the most extensively studied group of lipid kinases. These enzymes phosphorylate phosphoinositides at the 3-position of the inositol ring, producing the signaling molecule phosphatidylinositol-3,4,5-trisphosphate (PIP3). PIP3 activates downstream proteins, most notably the protein kinase AKT, which promotes cell growth, survival, and proliferation. Mutations in PI3K genes are frequently found in cancer.
Phosphoinositide 4-Kinases (PI4K)
PI4 kinases phosphorylate phosphatidylinositol at the 4-position and are essential for intracellular membrane trafficking and Golgi apparatus function.
Diacylglycerol Kinases (DGK)
Diacylglycerol kinases convert diacylglycerol (DAG), an important signaling molecule, into phosphatidic acid, thereby terminating DAG-dependent signaling. They play a role in immune cell activation.
Sphingosine Kinases (SphK)
Sphingosine kinases phosphorylate sphingosine to produce sphingosine-1-phosphate (S1P), a lipid mediator that regulates cell migration, survival, and inflammatory responses.
Lipid Kinases in Medicine
Due to their central role in cell biology, lipid kinases are highly relevant targets for the development of new therapeutic drugs. Dysfunction of lipid kinases has been linked to a variety of diseases:
- Cancer: Overactive PI3K signaling promotes uncontrolled cell growth. PI3K inhibitors (e.g., idelalisib, copanlisib) are already used in cancer therapy.
- Type 2 diabetes mellitus: Disruptions in the PI3K/AKT signaling pathway impair insulin sensitivity.
- Chronic inflammatory diseases: Lipid kinase pathways modulate inflammatory responses and are targets of immunosuppressive therapies.
- Autoimmune diseases: Selective inhibition of PI3K isoforms (e.g., PI3Kδ) is being investigated in rheumatic and hematologic conditions.
Diagnostic Relevance
Alterations in lipid kinase genes (mutations, amplifications) can be detected using molecular diagnostics such as next-generation sequencing (NGS) or immunohistochemistry. This is relevant to precision oncology, as the identification of specific mutations influences the choice of targeted therapy.
References
- Vanhaesebroeck B, Stephens L, Hawkins P. PI3K signalling: the path to discovery and understanding. Nature Reviews Molecular Cell Biology, 2012; 13(3):195–203.
- Wymann MP, Schneiter R. Lipid signalling in disease. Nature Reviews Molecular Cell Biology, 2008; 9(2):162–176.
- Fruman DA, Chiu H, Hopkins BD, et al. The PI3K Pathway in Human Disease. Cell, 2017; 170(4):605–635.
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