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Cell Transport and Homeostasis

Essay by   •  February 13, 2011  •  Research Paper  •  740 Words (3 Pages)  •  1,506 Views

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Cell Transport And Homeostasis

The roles of different types of cell-membrane proteins in the preservation of body organs donated for transplant is very vast. Certain cell-membrane proteins carry several different types of nutrients that are beneficial and are sometimes very important to keep organs that are to be transplanted healthy and fresh. Organic nutrients are some very good preservers.

One of the most transplanted organs is the kidney. It is important that this organ has nutrients because it can dry and rot rather quickly. These nutrients transfer energy from the cell membrane and transport it to the organ to keep it preserved. If the cell membrane lacks the proper internal structure that is beneficial to the organ, then that can be very harmful in the long run. It could also change the properties and internal structure of the organ that it is located in.

Another organ that is transplanted a lot is the heart. In my research, I found that hearts need to stay on ice as well as be neutralized by the nutrients in cell-membrane proteins. Without these things, as well as fast transportation, the heart can quickly harden and become useless. The proteins also need to learn how to adapt outside of their natural environment because they are not used to living in an organ that is not doing work in an organ system and body for a specific amount of time.

These proteins also require oxygen that, obviously, a transplanted organ doesn't have for a certain amount of time. If these proteins do not receive that oxygen, there is no good in the proteins because they cannot do their preservation job properly.

The different kinds of proteins include: Host-versus-graft reactions; Direct allorecognition Indirect allorecognition (used for all organs, especially during early post-transplant period, at any time post-transplant, and especially later on). Graft-versus-host reactions (Used for Liver, intestines, and lungs. Any organ recipient who also receives bone marrow cells). Microchimerism (tolerance) (used for Liver, any organ, especially after infusion with bone marrow cells HLA -restricted immune mechanisms) and Recurrent autoimmune disease (used with (viral) infections, liver, and kidney).

These are some of the conclusions drawn from an experiment that the American Heart Association, Inc. performed; study shows for the first time that exogenous proteins can be displayed on the endothelium of solid organs for therapeutic purposes. This approach provides a convenient and rapid means of displaying exogenous proteins on the surface of cells, tissues, and solid organs, with broad research and therapeutic implications. The critical role that the Fas/Fas ligand (FasL) interaction plays in immune homeostasis, self-tolerance, and immune privilege in vital organs led to attempts to use these molecules to prevent allograft rejection and induce tolerance to solid organ grafts. Conceptually, the presentation of alloantigens to T cells in the presence of FasL may lead to the apoptosis of activated cells and may block alloreactive responses. The process of activation-induced cell death (AICD) involves interaction of FasL with the Fas receptor expressed on the surface of activated lymphocytes, which initiates a cascade

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