LCE1a2

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LCE’s are consistent of 3 groups: LCE1, LCE2, and LCE3. The full display of the gene cluster can be found in figure 2. Research has found that LCE3B and LCE3C genes, is under regulation of psoriasis-associated Th1 and Th17 cytokines which is a strong indication of the way that the LCE3 cluster functions and attributes to the epidermal layer (Hanna Niehues). When it comes to the capabilities of LCE3 it has been found that LCE3 proteins cause a rapid killing which is reminiscent of the kinetics of killing by human neutrophil defensins where the outer and inner membrane of Escherichia coli are sequentially permeabilized within 30–60 minutes (Lehrer et al., 1989). In addition to this capability, it has also been found that LCE3 is primarily respondent to inflammation of the epidermal layer. As far as the other gene clusters such as LCE1 and LCE2 there has yet to be found research on those clusters and their potential specified capabilities. Predictions are that they respond in a similar way to LCE3 but may have a specified role in aiding in that inflammatory response. This is another major question within the realm of LCE’s. Are these gene clusters and even individual genes coded to respond to specific stimuli different from its cluster neighbors?
LCE’s are consistent of 3 groups: LCE1, LCE2, and LCE3. The full display of the gene cluster can be found in figure 2. Research has found that LCE3B and LCE3C genes, is under regulation of psoriasis-associated Th1 and Th17 cytokines which is a strong indication of the way that the LCE3 cluster functions and attributes to the epidermal layer (Hanna Niehues). When it comes to the capabilities of LCE3 it has been found that LCE3 proteins cause a rapid killing which is reminiscent of the kinetics of killing by human neutrophil defensins where the outer and inner membrane of Escherichia coli are sequentially permeabilized within 30–60 minutes (Lehrer et al., 1989). In addition to this capability, it has also been found that LCE3 is primarily respondent to inflammation of the epidermal layer. As far as the other gene clusters such as LCE1 and LCE2 there has yet to be found research on those clusters and their potential specified capabilities. Predictions are that they respond in a similar way to LCE3 but may have a specified role in aiding in that inflammatory response. This is another major question within the realm of LCE’s. Are these gene clusters and even individual genes coded to respond to specific stimuli different from its cluster neighbors?
As stated before, LCE’s are not restricted to the human genome. They are found in the mammalian community and their function is hypothesized to be about the same and just in different locations. “On human chromosome 1q21, a 2-Mb region called the epidermal differentiation complex comprises many genes encoding structural and regulatory proteins that are of crucial importance for keratinocyte differentiation and stratum corneum properties” (Henry, J 2012). Not only are LCE’s located here but a similar set of proteins are also present, and they are known as small proline-rich region proteins (SPRRs). These proteins are expected to hold very similar purposes as the ones housed in the LCE gene cluster. Not only that but its location is directly followed by the LCE location. Due to the proximity and similarity in these two epidermal components it only further pushes the idea that due to the position of LCE gene clusters, their functions can’t be too far off from each other.
As stated before, LCE’s are not restricted to the human genome. They are found in the mammalian community and their function is hypothesized to be about the same and just in different locations. “On human chromosome 1q21, a 2-Mb region called the epidermal differentiation complex comprises many genes encoding structural and regulatory proteins that are of crucial importance for keratinocyte differentiation and stratum corneum properties” (Henry, J 2012). Not only are LCE’s located here but a similar set of proteins are also present, and they are known as small proline-rich region proteins (SPRRs). These proteins are expected to hold very similar purposes as the ones housed in the LCE gene cluster. Not only that but its location is directly followed by the LCE location. Due to the proximity and similarity in these two epidermal components it only further pushes the idea that due to the position of LCE gene clusters, their functions can’t be too far off from each other.
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[[Image:lcechart.jpg]]
== LCE1a2 ==
== LCE1a2 ==

Revision as of 20:34, 23 April 2022

Structure

Caption for this structure

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References

  1. Hanson, R. M., Prilusky, J., Renjian, Z., Nakane, T. and Sussman, J. L. (2013), JSmol and the Next-Generation Web-Based Representation of 3D Molecular Structure as Applied to Proteopedia. Isr. J. Chem., 53:207-216. doi:http://dx.doi.org/10.1002/ijch.201300024
  2. Herraez A. Biomolecules in the computer: Jmol to the rescue. Biochem Mol Biol Educ. 2006 Jul;34(4):255-61. doi: 10.1002/bmb.2006.494034042644. PMID:21638687 doi:10.1002/bmb.2006.494034042644

Henry, J., Toulza, E., Hsu, C. Y., Pellerin, L., Balica, S., Mazereeuw-Hautier, J., Paul, C., Serre, G., Jonca, N., & Simon, M. (2012). Update on the epidermal differentiation complex. Frontiers in bioscience (Landmark edition), 17, 1517– 1532.https://doi.org/10.2741/401 Jackson, B., Tilli, C. M., Hardman, M. J., Avilion, A. A., MacLeod, M. C., Ashcroft, G. S., & Byrne, C. (2005). Late cornified envelope family in differentiating epithelia-response to calcium and ultraviolet irradiation. The Journal of investigative dermatology, 124(5), 1062–1070. https://doi.org/10.1111/j.0022202X.2005.23699.x Lehrer RI, Barton A, Daher KA, Harwig SS, Ganz T, Selsted ME. Interaction of human defensins with Escherichia coli. Mechanism of bactericidal activity. J Clin Invest. 1989;84:553–61. Moreci, R. S., & Lechler, T. (2020). Epidermal structure and differentiation. Current biology : CB, 30(4), R144–R149. https://doi.org/10.1016/j.cub.2020.01.004 Niehues, H., Tsoi, L. C., van der Krieken, D. A., Jansen, P., Oortveld, M., RodijkOlthuis, D., van Vlijmen, I., Hendriks, W., Helder, R. W., Bouwstra, J. A., van den Bogaard, E. H., Stuart, P. E., Nair, R. P., Elder, J. T., Zeeuwen, P., & Schalkwijk, J. (2017). Psoriasis-Associated Late Cornified Envelope (LCE) Proteins Have Antibacterial Activity. The Journal of investigative dermatology, 137(11), 2380– 2388. https://doi.org/10.1016/j.jid.2017.06.003

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Madison Thompson, Michal Harel

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