Collagen

From Proteopedia

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Revision as of 17:59, 10 January 2011

Collagen, the most abundant protein in vertebrates, is an extracellular, inextensible fibrous protein that comprises the major protein component of such stress-bearing structures as bones, tendons, and ligaments. As with all fibrous proteins collagen is, for the most part, characterized by highly repetitive simple sequence. Here we study two model compounds (The structure of 4CLG is shown in the applet to the right.) for naturally occurring collagen, in order to develop an understanding of the fibrous portion of collagen and to show how the different levels of protein structure come together and form a highly ordered and stable fiber. Collagen's properties of rigidity and inextensibility are due to this highly ordered structure. The part of collagen without structural order is not illustrated in this model. This part of the protein complex having a different amino acid composition, lysine and hydroxylysine are particularly important residues, is globular in nature and not as structurally organized. Lysine and hydroxylysine form covalent crosslinks in the protein complex, thereby adding strength and some flexibility to the fiber. This covalent crosslinking continues throughout life and produces a more rigid collagen and brittle bones in older adults. Go to Collagen Structure & Function for information on the functions and disorders of collagen and a link in the External Links section of this page for assembly movies of the triple helix of types I and IV.

Structure of a Segment

A fiber segment is made up of 5 tropocollagens, each is shown in a . One limitation of this model of collagen segment is that instead of having flush cut ends as shown here, the ends of the tropocollagen in an actual fiber section would be . When the tropocollagens come together to form the fiber segment, they actually overlap one another in a staggered pattern. The presents of these staggered ends permit the tropocollagens from different segments to associate, and this associations result in the formation of a strong fiber. Add tropocollagens at a time to form the fiber section, , , , . View fiber segment as . Viewing the segment from the end one can see that without the side chains being displayed the center of the fiber is empty. Each contains 3 parallel peptide chains wrapped around one another to make a right-handed triple helix that is 87 Å long and ~10 Å in diameter. Tropocollagen displayed as only.

Lower Levels of Structure

Primary Structure of Peptide

of the peptide in wireframe display. Identify the amino acids making up the peptide by resting the cursor on a residue and observing the name in the label (Toggling spin off will make this easier.). Which three amino acids are present in the peptide in a reocurring pattern? Collagen is characterized by a distinctive repeating sequence: (Gly-X-Y)n where X is often Pro, Y is usually 5-hydroxyproline (Hyp), and n may be >300. The model (4CLG) being studied here contains a of residues - Gly-Pro-Hyp. This sequence produces a conformation which is a with a pitch (rise per turn) of 10.0 Å and a rise which gives , the peptide is colored in three residue segments. the center axis of a segment of the helix. Since a helix with a larger rise is superimposed on the helix described above, the entire center axis does not align for viewing. The rise for the α helix is 3.6. The shows that the psi and phi angles of the collagen helix are different from the α-helix. The two clusters shown here are outside of the area expected for an α-helix. Review where you would expect a cluster of α-helix residues to be located.

Other Levels of Structure

As shown above tropocollagen is formed by twisting around each other, and in doing so the peptides make (Cyan colored residues mark the approximate length of one turn.). mark the approximate distance of one turn in a tropocollagen. Tropocollagen displayed as clearly shows both types of helical turns - the 3.3 residue/turn and ~21 residue/turn. Looking down the axis of a tropocollagen displayed as wireframe, glycine can be seen of the triple helix. The two types of helical turns consistently positions the Gly in the center of the triple helix. Proline and the hydroxyproline are on the of the triple helix. With the hydroxyl group of Hyp extending to the surface of the triple helix, it can be involved in hydrogen bond formation, as will be seen in the next section. The primary structure of repeating Gly-Pro-Hyp along with the two types of helical turns determine the 3D positions of Gly, Pro and Hyp in the tropocollagen.

In order to make a compact strong fiber the interior residues of the triple helix need to be close packed. The is the only one small enough to accommodate this close packing in the interior of the triple helix. (Realize that in this model the hydrogen on the α carbon is not displayed.) , one on each of three different chains, are close packed together. The gray atoms of the yellow and lime Gly are the α-carbons, and only a hydrogen could fit between these carbons and the atoms of the adjacent Gly. on each of the 3 chains are shown close packed to the three Gly (lime, cyan, yellow). Adding the shows that Pro and Hyp are tightly positioned around the small interior Gly.

Maintainance Forces

Intra-tropocollagen Attractions

Intra-tropocollagen attractions are primarily hydrogen bonds formed between the peptides in the triple helix. The three polypeptide chains are in position by one residue, that is, a Pro on Chain A is at the same level along the triple helix axis as a Gly on Chain B and a Hyp on Chain C. This staggered arrangement not only a Gly main chain NH (imino group) with a Pro main chain O (carbonyl oxygen) on one of the other peptides but also brings the two groups close enough to form between the imino hydrogen and the carbonyl oxygen. This alignment of Gly occurs with each of the three peptides so that the Gly hydrogen of Chain A forms a (orange) with the Pro carbonyl oxygen on Chain B, and likewise Gly of (yellow) and Gly of (green). The force of these hydrogen bonds extending the length of the tropocollagen add up to a strong attractive force which mantain the integrity of the tropocollagen. Since the main chain N atoms of both Pro and Hyp residues lack H atoms, only Gly can provide hydrogen to form these hydrogen bonds.

Inter-tropocollagen Attractions

Hydrogen bonds are also an important inter-tropocollagen force which holds the tropocollagens together in the fiber segment. These hydrogen bonds are formed between the hydroxy hydrogen of a Hyp which, as see above, is a residue on the of the triple helix and a backbone carbonyl oxygen. The hydroxyl groups are the atoms that extend out the most from the center of the triple helical structure. As the peptides in a tropocollagen twist about each other they come into from peptides in adjacent tropocollagens. The two peptide highlighted in spacefill are located in two different tropocollagens. Notice that they make contact with each other in the middle of the strands, and a hydrogen bond is located at this point of contact. The consist of the oxygen of a carbonyl of a Hyp in a peptide of one tropocollagen and the hydroxyl hydrogen of a Hyp in a peptide of another tropocollagen. Another example shows from two different tropocollagens making contact at the ends of the fiber segment, and of course it is within these regions where the inter-tropocollagen attractions occur. At one end a is formed between a hydrogen of Hyp in one peptide and an oxygen of a Gly carbonyl in the second peptide. At the other end of the two peptides a donates its electrons to a Hyp hydroxyl hydrogen. Show the in the context of the six peptides of the two tropocollagens. The above examples of hydrogen bonding illustrate that Hyp plays a central role in maintaining the structures of both the tropocollagen and the collagen fiber.

Effect of a Mutation

The mutation being considered is an Ala replacing a Gly. Synthetic model PDB ID: 1CAG is whose peptides contain thirty residues and have a of (Pro-Hyp-Gly)4-Pro-Hyp-Ala-(Pro-Hyp-Gly)5 (Ala displayed as large wireframe and colored as C O N). Viewing 1CAG from the side of the fiber shows: the is only partially visible because it is buried in the interior, being much more visible is positioned closer to the surface, being entirely on the surface is clearly visible, and being a substitute for Gly is only partially visible.

The of the tropocollagen is shown with the Ala appearing as olive and the Pro and Hyp adjacent to the Ala appearing as dark brown. Notice that the surface at these Pro and Hyp bulges slightly. This protrusion is due to the fact that the packing about the Ala side chains is not as close as it is about the Gly. In the two side-by-side scenes shown below compare the amount of open space between the chains in the area of the scene center. In the 1CAG scene in the area of the Ala the distance between the chains is slightly greater than that of 4CLG scene.

Gly Packing in 4CLG.PDB ()

Ala Packing in 1CAG.PDB (Mutated Collagen) ()

With show the Gly displayed as spacefill and with show Ala displayed as spacefill. There is more open space between the spacefilled Ala (yellow) (1CAG.PDB) than between the spacefilled Gly of 1CAG and the non-mutated model (4CLD.PDB). After adding Pro to the spacefill display of and this openness permits sections of the black background to appear in the mutated model, but not in the model that contain only Gly. The open sections in the area of the Ala are also visible after adding Hyp to the spacefill display of and . These conformational changes, which are due to the substitution of Ala for Gly and disrupt collagen's rope-like structure, are responsible for the symptoms of such human diseases as osteogenesis imperfecta and certain Ehlers-Danlos syndromes.

Collagen Backbone and the Effect of a Mutation

(KineMage currently not supported) This kinemage displays all of the atoms of the collagen model compound (Pro-Hyp-Gly)4-Pro-Hyp-Ala-(Pro-Hyp-Gly)5 in stick form (note that the "essential" Gly residue in this model compound's central triplet is replaced by Ala). View1 shows the triple helix in side view with "Chain 1" in pinktint, "Chain 2" in yellowtint, and "Chain 3" in white. The Pro, Hyp, and Ala side chains, which are independently controlled by the corresponding buttons, are green, cyan, and magenta, respectively. Use View1 and View2, which is down the triple helix axis, to prove to yourself that all Pro and Hyp side chains are on the periphery of the triple helix. These rigid groups are thought to help stabilize the collagen conformation.

View3 and View4 are side and top views of a segment of the collagen helix in which its three polypeptides all consist of repeating triplets of ideal sequence, (Gly-Pro-Hyp)n. Go to View3 to see that the three polypeptide chains are staggered in sequence by one residue, that is, a Gly on Chain 1 is at the same level along the triple helix axis as a Hyp on Chain 2 and a Pro on Chain 3. Turn on the "H bonds" button (H bonds are represented by dashed orange lines), to see that this staggered arrangement permits the formation of a hydrogen bond from the Gly main chain NH of Chain 1 to the Pro main chain O on Chain 2 (and likewise from Chain 2 to Chain 3 and from Chain 3 to Chain 1). Since the main chain N atoms of both Pro and Hyp residues lack H atoms, this exhausts the ability of the main chain to donate hydrogen bonds. Although the center of the triple helix appears to be hollow in View4, taking into account the van der Waals radii of its various atoms reveals that the center of the triple helix is, in fact, quite tightly packed. Indeed, the above hydrogen bonds pass very close to the center of the triple helix. This close packing accounts for the absolute requirement for a Gly at every third residue in a functional collagen molecule. Since, as you can see, the Gly Ca atoms are near the center of the triple helix, the side chain of any other residue at this position would, as we shall see below, significantly distort and hence destabilize the collagen triple helix.

View5 and View6 show the side and top views of the triple helix segment containing an Ala on each chain instead of a Gly. The effect of replacing the Gly H atom side chain with a methyl group to form Ala, the smallest residue substitution possible, is quite striking. The interior of the collagen triple helix is too crowded to accommodate an Ala side chain without significant distortion. The triple helix in this region therefore unwinds and expands so that no H-bonds form in this region. The unwinding of the triple helix in the region about the Ala residues is, perhaps, best seen by returning to KINEMAGE above this one. You can see that the triple helix is bulged out in the center of View1. These conformational changes, which disrupt collagen's rope-like structure, are responsible for the symptoms of such human diseases as osteogenesis imperfecta and certain Ehlers-Danlos syndromes.

Exercise in large part by John H. Connor (present address: Department of Microbiology, Boston University School of Medicine, 850 Harrison Ave, Boston, MA, 02118, USA)

External Links

Movies of assembly of triple helix of type I and IV collagen.

Proteopedia Page Contributors and Editors (what is this?)

Karl Oberholser, Alexander Berchansky, Michal Harel, Ala Jelani, Jaime Prilusky, Eric Martz, Eran Hodis, David Canner, Judy Voet, Tilman Schirmer

Retrieved from "http://52.214.119.220/wiki/index.php/Collagen"

@@ Line 32: / Line 32: @@
 The mutation being considered is an Ala replacing a Gly.  Synthetic model PDB ID: [[1CAG]] is <scene name='Collagen/1cag/7'>tropocollagen</scene> whose peptides contain thirty residues and have a <scene name='Collagen/Collagen_chain_1cag/4'>sequence</scene> of (Pro-Hyp-Gly)4-Pro-Hyp-Ala-(Pro-Hyp-Gly)5 (Ala displayed as large wireframe and colored as {{Template:ColorKey_Element_C}} {{Template:ColorKey_Element_O}} {{Template:ColorKey_Element_N}}).    Viewing 1CAG from the side of the fiber shows: the <scene name='Collagen/1cag1/1'>Gly</scene> is only partially visible because it is buried in the interior, <scene name='Collagen/1cag2/1'>Pro</scene> being much more visible is positioned closer to the surface, <scene name='Collagen/1cag3/1'>Hyp</scene> being entirely on the surface is clearly visible, and <scene name='Collagen/1cag4/1'>Ala</scene> being a substitute for Gly is only partially visible.
-The <scene name='Collagen/1cag_surface/4'>surface</scene> of the tropocollagen is shown with the Ala appearing as olive and the Pro and Hyp adjacent to the Ala appearing as dark brown.  Notice that the surface at these Pro and Hyp bulges slightly.  This protrusion is due to the fact that the packing about the Ala side chains is not as close as it is about the Gly.  This difference in the packing can be seen in the two side-by-side scenes shown below.  There is more open space between the Ala (yellow) (1CAG.PDB) than between the Gly of 1CAG and the non-mutated model (4CLD.PDB).
+The <scene name='Collagen/1cag_surface/4'>surface</scene> of the tropocollagen is shown with the Ala appearing as olive and the Pro and Hyp adjacent to the Ala appearing as dark brown.  Notice that the surface at these Pro and Hyp bulges slightly.  This protrusion is due to the fact that the packing about the Ala side chains is not as close as it is about the Gly.  In the two side-by-side scenes shown below compare the amount of open space between the chains in the area of the scene center.  In the 1CAG scene in the area of the Ala the distance between the chains is slightly greater than that of 4CLG scene.
 </StructureSection>
-<table width='100%' align='left' cellpadding='5'><tr><td rowspan='2'>&nbsp;</td><td bgcolor='#eeeeee'><Structure load='4CLG' size='510' frame='true' align='left' name='id1' scene='Collagen/Glys_close_pack2/1' /></td><td bgcolor='#eeeeee'><Structure load='1CAG' size='510' frame='true' align='right' name='id2' scene='Collagen/1cag_ala_pack2/2' /></td></tr><tr><td bgcolor='#eeeeee'><center>'''Gly Packing in 4CLG.PDB'''&nbsp;(<scene name='Collagen/Glys_close_pack2/1'> Initial scene</scene>)</center></td><td bgcolor='#eeeeee'><center>'''Ala Packing in 1CAG.PDB (Mutated Collagen)'''&nbsp;(<scene name='Collagen/Glys_close_pack2/1'> Initial scene</scene>)</center></td></tr></table>
+<table width='100%' align='left' cellpadding='5'><tr><td rowspan='2'>&nbsp;</td><td bgcolor='#eeeeee'><Structure load='4CLG' size='510' frame='true' align='left' name='id1' scene='Collagen/Glys_close_wf/1' /></td><td bgcolor='#eeeeee'><Structure load='1CAG' size='510' frame='true' align='right' name='id2' scene='Collagen/1cag_ala_pack_wf/1' /></td></tr><tr><td bgcolor='#eeeeee'><center>'''Gly Packing in 4CLG.PDB'''&nbsp;(<scene name='Collagen/Glys_close_pack2/1'> Initial scene</scene>)</center></td><td bgcolor='#eeeeee'><center>'''Ala Packing in 1CAG.PDB (Mutated Collagen)'''&nbsp;(<scene name='Collagen/Glys_close_pack2/1'> Initial scene</scene>)</center></td></tr></table>
 __NOTOC__
-After adding <font color='tomato'>Pro</font> to the spacefill display of <scene name='Collagen/Glys_pro_close2/1' target='id1'>4CLG</scene> and <scene name='Collagen/1cag_ala_pro_pack/1' target='id2'>1CAG </scene> this openness permits sections of the black background to appear in the mutated model, but not in the model that contain only Gly.  These sections of background in the area of the Ala are also visible after adding <font color='limegreen'>Hyp</font> to the spacefill display of <scene name='Collagen/Glys_pro_hyp_close2/1' target='id1'>4CLG</scene> and <scene name='Collagen/1cag_ala_pro_hyp_pack/1' target='id2'>1CAG</scene>. These conformational changes, which are due to the substitution of Ala for Gly and disrupt collagen's rope-like structure, are responsible for the symptoms of such human diseases as osteogenesis imperfecta and certain Ehlers-Danlos syndromes.
+With <scene name='Collagen/Glys_close_pack2/1' target='id1'>4CLG</scene> show the Gly displayed as spacefill and with <scene name='Collagen/1cag_ala_pack2/2' target='id2'>1CAG</scene> show Ala displayed as spacefill.  There is more open space between the spacefilled Ala (yellow) (1CAG.PDB) than between the spacefilled Gly of 1CAG and the non-mutated model (4CLD.PDB).  After adding <font color='tomato'>Pro</font> to the spacefill display of <scene name='Collagen/Glys_pro_close2/1' target='id1'>4CLG</scene> and <scene name='Collagen/1cag_ala_pro_pack/1' target='id2'>1CAG </scene> this openness permits sections of the black background to appear in the mutated model, but not in the model that contain only Gly.  The open sections in the area of the Ala are also visible after adding <font color='limegreen'>Hyp</font> to the spacefill display of <scene name='Collagen/Glys_pro_hyp_close2/1' target='id1'>4CLG</scene> and <scene name='Collagen/1cag_ala_pro_hyp_pack/1' target='id2'>1CAG</scene>. These conformational changes, which are due to the substitution of Ala for Gly and disrupt collagen's rope-like structure, are responsible for the symptoms of such human diseases as osteogenesis imperfecta and certain Ehlers-Danlos syndromes.