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T Cells  
  
1089   03:46 مساءاً   date: 1-11-2015
Author : Beck, Gregory, and Gail S. Habicht
Book or Source : Immunity and the Invertebrates
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Date: 1-11-2015 1090
Date: 6-11-2015 4358
Date: 8-11-2015 2934

T Cells

Vertebrate animals have two immune system mechanisms to specifically identify and remove infectious agents from the body. In humoral immunity, proteins called antibodies bind to the foreign invader, targeting it for de­struction by nonspecific defenses. In cell-mediated immunity, immune cells directly attach to and destroy the invader. Both mechanisms require the ac­tions of T cells.

T cells belong to a category of white blood cells called lymphocytes. Lymphocytes are slightly larger than red blood cells and are found in the blood, lymphatic organs, and many other structures in the body. The spleen, lymph nodes, and tonsils are examples of lymphatic organs. Lymphocytes have large, round nuclei that take up almost all of the space inside the cell. Other examples of lymphocytes include B cells and natural killer cells.

Like all blood cells, T cells are made in the bone marrow. The T is an abbreviation for the word “thymus,” an organ found on the front of the tra­chea, near the lungs and heart. After T cells are made, they go to the thy­mus to become mature. Three important events occur in the thymus.

First, each T cell begins to produce a protein called a receptor on its cell surface. T cell receptors recognize antigens, which are molecules that can start an immune response. Foreign invaders are made of many antigens. An antigen can fit inside the T cell receptor much like a key fitting into a lock. Each T cell receptor recognizes only one type of antigen. This ex­plains how the immune system specifically identifies foreign invaders.

As a T cell matures, the genes that contain the information on how to build the T cell receptor are rearranged. Millions of possible T cell receptors can be produced by this rearrangement. However, once the genes are re­arranged, a given T cell is committed to making only one type of receptor.

Unfortunately, some T cells express receptors that can recognize and damage the body’s own antigens. Consequently, the second event that   occurs in the thymus is the destruction of these T cells. This process is called clonal deletion. The surviving T cells can roam through the body’s organs, searching only for invaders.

Scanning electron micrograph of three T cells.

The third event that occurs before the T cells leave the thymus results in the production of T cells with different functions. Some of the T cells will produce a surface protein called CD4. These T cells are called helper T cells (Th cells), T4 cells, or CD4 cells. As their name implies, TH cells assist other immune cells. Other T cells in the thymus produce a surface protein called CD8. These T cells are called cytotoxic T cells (TC cells), T8 cells, or CD8 cells. As their name implies, TC cells destroy foreign in­vaders. Some CD8 cells seem to be able to control the immune system and are consequently called suppressor T cells.

TH cells function in both humoral immunity and cell-mediated immu­nity. If foreign antigens enter the body, cells called antigen-presenting cells (APCs) engulf the antigen and attach it to a molecule called a class II ma­jor histocompatibility complex (MHC) protein. The antigen and class II MHC protein are then moved to the surface of the APC. The APC pre­sents these molecules to a series of TH cells with different receptors. If there is a match between a TH cell receptor and the antigen, the TH cell is stim­ulated to divide rapidly and produce chemicals called cytokines. The CD4 molecule on the TH cell connects with the class II MHC protein on the APC to stabilize the cell-to-cell connection and provide additional signals. There are many other molecules on the surfaces of these cells that must in­teract, showing the complexity of the process.

In humoral immunity, stimulated TH cells activate B cells. Like APCs, B cells bring foreign antigens inside and then display them with class II MHC proteins on the surface. The stimulated TH cells then attach to the B cells just as they did with the APCs. This contact, along with the cytokines, stimulates the B cell to divide rapidly, and it produces antibodies. Antibod­ies can clear other copies of the foreign invader from the body.

TH cells interact with B cells and TC cells to protect the body from infection.

In cell-mediated immunity, stimulated TH cells activate TC cells. All cells of the body produce surface proteins called class I MHC proteins. If the cell is abnormal (cancerous or infected with a virus), the abnormal anti­gen is displayed with the class I MHC protein. A TC cell with the match- ing receptor will recognize the abnormal cell. The TC cell receptor binds to the abnormal antigen and the CD8 molecule binds to the class I MHC molecule. The TC cell receives other signals from cytokines made by TH cells. Now the TC cell divides rapidly and searches for other abnormal cells. When the TC cells find abnormal cells, they bind to them and release chem­icals that destroy the target cell. Perforin, lymphotoxin, and tumor necro­sis factor are examples of these chemicals. Both B cells and TC cells can become memory cells. Memory cells eliminate an invader more quickly if it appears again.

Th cells also aid nonspecific immunity by producing cytokines that cause inflammation and attract and activate white blood cells such as neutrophils, natural killer cells, and macrophages to the site of infection.

T cells may function abnormally, causing a variety of medical problems. For example, human immunodeficiency virus infects and destroys TH cells. Consequently, many TC cells and B cells are not activated. The invader gets the upper hand, and the body cannot easily rid itself of the infection or ab­normal cell.

Sometimes TC cells overreact to a harmless antigen and damage healthy tissue. This is what happens in individuals with allergies to poison ivy, la­tex, cosmetics, and metals. TC cells are also responsible for the rejection of a transplanted organ.

References

Beck, Gregory, and Gail S. Habicht. “Immunity and the Invertebrates.” Scientific American 275, no. 5 (1996): 60-65.

Friedlander, Mark P., Jr., and Terry M. Phillips. The Immune System: Your Body’s Disease-Fighting Army. Minneapolis, MN: Lerner Publications Company, 1998.

National Institutes of Health. Understanding the Immune System. Washington, DC: National Institutes of Health, 1993.

Nossal, Gustav J. “Life, Death, and the Immune System.” Scientific American 269, no. 3 (1993): 53-62.

Paul, William E. “Infectious Diseases and the Immune System.” Scientific American 269, no. 3 (1993): 90-97.




علم الأحياء المجهرية هو العلم الذي يختص بدراسة الأحياء الدقيقة من حيث الحجم والتي لا يمكن مشاهدتها بالعين المجرَّدة. اذ يتعامل مع الأشكال المجهرية من حيث طرق تكاثرها، ووظائف أجزائها ومكوناتها المختلفة، دورها في الطبيعة، والعلاقة المفيدة أو الضارة مع الكائنات الحية - ومنها الإنسان بشكل خاص - كما يدرس استعمالات هذه الكائنات في الصناعة والعلم. وتنقسم هذه الكائنات الدقيقة إلى: بكتيريا وفيروسات وفطريات وطفيليات.



يقوم علم الأحياء الجزيئي بدراسة الأحياء على المستوى الجزيئي، لذلك فهو يتداخل مع كلا من علم الأحياء والكيمياء وبشكل خاص مع علم الكيمياء الحيوية وعلم الوراثة في عدة مناطق وتخصصات. يهتم علم الاحياء الجزيئي بدراسة مختلف العلاقات المتبادلة بين كافة الأنظمة الخلوية وبخاصة العلاقات بين الدنا (DNA) والرنا (RNA) وعملية تصنيع البروتينات إضافة إلى آليات تنظيم هذه العملية وكافة العمليات الحيوية.



علم الوراثة هو أحد فروع علوم الحياة الحديثة الذي يبحث في أسباب التشابه والاختلاف في صفات الأجيال المتعاقبة من الأفراد التي ترتبط فيما بينها بصلة عضوية معينة كما يبحث فيما يؤدي اليه تلك الأسباب من نتائج مع إعطاء تفسير للمسببات ونتائجها. وعلى هذا الأساس فإن دراسة هذا العلم تتطلب الماماً واسعاً وقاعدة راسخة عميقة في شتى مجالات علوم الحياة كعلم الخلية وعلم الهيأة وعلم الأجنة وعلم البيئة والتصنيف والزراعة والطب وعلم البكتريا.




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