المرجع الالكتروني للمعلوماتية
المرجع الألكتروني للمعلوماتية

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Untitled Document
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Golgi  
  
3067   04:35 مساءاً   date: 19-10-2015
Author : Balch W. E., and B. A. Bernard
Book or Source : Protein Sorting by Directed Maturation of Golgi
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Date: 20-10-2015 2285
Date: 1-11-2015 2000
Date: 26-10-2015 2916

Golgi

The Golgi (pronounced GOL-jee) complex (or Golgi apparatus or Golgi body) was discovered by Camillo Golgi (1844-1926), an Italian physician. While Dr. Golgi was staining neurons with silver nitrate (Golgi stain), he noticed small intracellular structures made up of vesicles and fibers known today as the Golgi complex.

Structure

The Golgi complex is composed of several layers of cisternae (fluid-filled membrane sacs) arranged like stacked pancakes near the outer edges of the endoplasmic reticulum (ER) near the nucleus. The Golgi complex is or­ganized into three biochemically distinct compartments: the cis Golgi, the medial Golgi, and trans Golgi; the cis Golgi is closest to the ER.

The intracellular structures known at the Golgi complex are involved in protein processing and secretion.

Protein Processing

The primary function of the Golgi complex is to modify, process, and sort newly produced proteins that arrive from the ER. These modifications in­clude adding or deleting specific sugar molecules to modify the branched sugar structures found on newly formed proteins. For example, some of the mannose sugars are cut from the oligosaccharide branch in the cis Golgi. Upon completion of this step, the protein travels to the medial Golgi where other sugars like N-acetylglucoseamine and fucose are added to the oligosac­charide branches on the protein. Further modifications to the carbohy­drates are completed in the trans Golgi. Carbohydrate additions may aid in the stability, transport, and/or function of the proteins.

Transport

Two models have been proposed to explain how newly produced proteins travel from the ER to the Golgi complex and travel among Golgi stacks. One model suggests that proteins are transported enclosed in vesicles. An­other model proposes that one stack of the Golgi “matures” into the next stack. This is called the cisternal progression model. Regardless of whichto their original stacks. Each of the vesi­cles that travel between the ER and Golgi stacks is coated with proteins that have “addressing tags” on them. For example, the vesicle that buds off of the ER has coat proteins that specifically direct it to the cis Golgi instead of the medial Golgi or some other organelle. Sometimes, enzymes and pro­teins that reside in the ER accidentally get caught in a vesicle going to the Golgi. When this happens, they return (retrograde transport) from the cis Golgi back to the ER in a vesicle coated with different proteins that are ad­dressed to the ER. Therefore, the Golgi has two sets of vesicles flowing in opposite directions. The first set of vesicles are filled with newly made pro­teins awaiting further modifications traveling in a forward or anterograde direction. The second set of vesicles are filled with enzymes and matured proteins seeking their resident organelle traveling in the reverse or retro­grade direction.

The Trans-Golgi Network (TGN)

The trans-Golgi network (TGN) is an extension of the trans Golgi where different types of vesicles are formed. The TGN can be thought of as a ma­jor protein sorting station inside the cell. Proteins maturing in the Golgi are sorted in the TGN for transport to several locations in the cell de­pending upon the biochemical tags that are found on the individual pro­teins. It is thought that proteins in the TGN are concentrated by linking up with receptor molecules in the lumen of the TGN. As proteins find their proper receptors, they may aggregate in one or few locations within the TGN and then bud off to form immature secretory vesicles: (1) secretory granules (vesicles that undergo further maturation and sorting of special­ized cargo); (2) secretory vesicles targeted to the plasma membrane; and (3) vesicles carrying degradative enzymes to lysosomes (small, acidic organelles that degrade macromolecules). Some selectivity and sorting of proteins may exist in these secretory vesicles before they get to the plasma mem­brane.

First, secretory vesicles are packaged with a high concentration of a spe­cific protein that has been transported to the TGN. For example, endocrine cells produce large amounts of specialized proteins called hormones that are packaged into secretory granules. When endocrine cells receive the cor­rect “signal” that triggers fusion of the secretory granules with the plasma membrane, these proteins are released into the circulatory system.

Second, some proteins are produced and secreted in a constitutive or constant manner; these proteins do not rely on extracellular signals for release and are not sorted to secretory granules. Instead, constitutive secretion involves vesicles originating at the TGN and traveling directly to the plasma membrane for exocytosis.

Finally, the TGN is a sorting station for the delivery of degradative en­zymes to lysosomes, vesicles containing nutrients that originated outside of the cell. Cells need to target these proteins to acidic lysosomes to assist in the digestion of internalized nutrients. Proteins destined for the lysosome have been modified with a unique sugar called mannose 6-phosphate. These lysosomal proteins are sorted in the TGN by binding to the mannose 6- phosphate receptor that then buds off in a vesicle that fuses with a lysosome. The low pH in the lysosome causes the mannose 6-phosphate bearing pro­tein to dissociate from the receptor. The empty receptor buds off from the lysosome in a small vesicle and is recycled to the TGN.

The Golgi complex plays an essential role in the sorting and targeting of proteins to various parts of the cell. Despite what is known, there are still many unanswered questions concerning the exact mechanisms involved with sorting and transporting cellular cargo throughout the cell. This is an im­portant area of investigation since many diseases such as I cell disease, Alzheimer Disease, Batten’s disease, and a host of other protein and lipid storage diseases are a result of cells missorting protein and lipids to the wrong locations in the cell.

References

Balch W. E., and B. A. Bernard. “Protein Sorting by Directed Maturation of Golgi.




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.