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P3 peptide

January 19, 2024

p3 peptide also known as amyloid β- peptide (Aβ)17–40/42 is the peptide resulting from the α- and γ-secretase cleavage from the amyloid precursor protein (APP). It is known to be the major constituent of diffuse plaques observed in Alzheimer's disease (AD) brains and pre-amyloid plaques in people affected by Down syndrome. However, p3 peptide's role in these diseases is not truly known yet.[2]

Representation of the 3D structure of p3 peptide.[1]

Structure edit

There is little information related to the p3 peptides composition and structure, and moreover most of it has to do with characteristics that concern to its role in Alzheimer's disease. p3 can be found as a 24 or 26 residues peptide, depending on which is gamma secretase's cleavage. The peptide which has 26 residues, presents the following sequence:

  • VFFAEDVGSNKGAIIGLMVGGVVIAT[3]

In relation to the secondary structure of p3 peptide, it is thought that after the cleavage by the α- and γ- secretases and extraction from the membrane it would convert quickly from the α-helix conformation it has when it is part of APPsα sequence to a β-hairpin structure. Then, this highly hydrophobic monomer would rapidly evolve into fibrils with no soluble intermediate forms, the ones related to amyloid’s structure. The main reason why p3 does not aggregate in amyloidogenic forms while does, is that the N-terminal domain1–16, which is present in Aβ’s sequence but not in p3's one, is known to protect the hydrophobic core of the oligomers from being dissolved by the watered medium. So, p3 peptide oligomers would likely expose hydrophobic residues to water and would be less stable. As a consequence, p3 peptide structural determinants can assemble into fibrils, but no oligomeric forms have been identified. That is why p3 peptide represents the benign form of amyloid.[4]

Properties edit

Energy plays a very important role in p3 peptides. While models have a strong negative energy, p3 oligomeric models have a positive one. Another characteristic that must be pointed out is that p3 peptides have more solvent-exposed hydrophobic surfaces (60%) than Aβ oligomers do (20%), so buried surface areas are not as big within p3 oligomers (30%) as they are within Aβ oligomers. These evidences show that the expected energy of the Aβ-based oligomeric models of p3 is always positive and that these models expose hydrophobic patches to the solvent and bury a small proportion of their accessible surface within the oligomeric intermediates. Having these facts into account, we can state that p3 oligomers' existence is thermodynamically unfavourable, which suggests that the p3 peptide cannot form stable soluble oligomers in the same way Aβ does. Solution of p3 cannot assemble into stable oligomers as Aβ1–42 in the same concentration does. Therefore, it is very possible that p3 could not last long by itself, evolving rapidly into fibrillar forms that hide exposed hydrophobic patches.[4]

p3 peptides have been analyzed in some researches with Western blot techniques. Primary antibodies were used to recognize Aβ1–16 residues. Unexpectedly, it was discovered that the residues did not show any signal. This confirms the absence of N-terminal domain Aβ1-16 in p3 peptides.[4]

Synthesis edit

p3 peptide generates from the 17-40 or 17-42 sequence of the amyloid precursor protein (APP), which is a type I integral membrane protein concerned in neurons’ synapses in many human tissues. Under normal physiological conditions, APP is processed with three different proteolytic enzymes: α-, β- and γ-secretases. At first, APP molecule is cut by α-secretase or β-secretase, and it will produce two different molecules for each case. These products are respectively APPsα or α-CTFs, when cut by α-secretase, or APPsβ and β-CTFs, when processed by β secretase. APPs derivates are sent both to the extra-cell, while CTFs rest anchored to the plasmatic membrane. Then, α- and β-CTFs are processed by γ-secretase, resulting the peptides p3 and respectively and releasing in both cases a cytoplasmic peptide fragment known as the APP intracellular domain (AICD). Both p3 and Aβ are sent to the extracellular medium.[4]

 
APP molecular processing and its different products. One of them is p3 peptide, which is sent to the extracellular medium.[1]

Role in Alzheimer’s disease and Down syndrome edit

 
p3 peptide is a product of non-amyloidogenic APP processing.

p3 peptide is known to have a role in AD and DS, however it has not been clearly determined yet.

In order to study the function of p3 peptide in AD, specific antibodies’ location techniques have been used to determine its absence or sparseness in aged non-AD brains. As it turns out, p3 peptide is prevalent in selected areas of AD brain in diffuse deposits and in a subset of dystrophic neuritis, both located in the temporal lobe limbic system.[5]

Although p3 peptide can assemble into fibrillar aggregates, its hydrophobic properties make it unable to rest in oligomeric forms. This might explain why p3 has no impact on synaptic function and therefore in AD, since it is a non-amyloidogenic product of APP.[4]

Despite this fact, p3 has been proved to have a role in formation of non-fibrillar deposits or lesions associated with DS, another neurological disorder that progresses at a faster rate than AD. Accordingly, DS patients have three copies of the APP gene, as they have three copies of the chromosome 21, so APP is overexpressed in the brain and AD develops at an early age. The disruption of the normal function of APP in AD and, consequently, in DS, including overexpression or altered processes, is the most likely explanation for amyloid plaque formation and subsequent neuronal loss and dementia, associated to memory, spatial disorientation and deterioration of intellectual capacity.[2]

Since p3 has not been studied deeply, there are different opinions about its role in brain.

P3 peptides are thought to have a role in neuronal death and in the enhanced inflammatory response in AD and DS, as it has been demonstrated that the treatment of cells with the p3 fragment, induced by the c-Jun N-terminal kinases (JNK) phosphorylation, is involved in neuronal cells apoptosis and causes the death of SH-SY5Y and IMR‐32 human neuroblastoma cells.[6]

References edit

  1. ^ a b PDB: 3MOQ
  2. ^ a b McCandless, Gregory T. (2008). (MS Thesis). Louisiana State University. OCLC 315888712. Archived from the original on 2013-10-29. Retrieved 2013-10-22.[page needed]
  3. ^ "Sequence Search: VFFAEDVGSNKGAIIGLMVGGVVIAT". Protein Data Bank.[permanent dead link]
  4. ^ a b c d e Dulin F, Léveillé F, Ortega JB, Mornon JP, Buisson A, Callebaut I, Colloc'h N (2008). "p3 peptide, a truncated form of Aβ devoid of synaptotoxic effect, does not assemble into soluble oligomers". FEBS Letters. 582 (13): 1865–70. doi:10.1016/j.febslet.2008.05.002. PMID 18474239. S2CID 43078358.
  5. ^ Higgins LS, Murphy GM, Forno LS, Catalano R, Cordell B (1996). "p3 β-Amyloid Peptide Has a Unique and Potentially Pathogenic Immunohistochemical Profile in Alzheimer's Disease Brain". The American Journal of Pathology. 149 (2): 585–96. PMC 1865300. PMID 8701997.
  6. ^ Wei W, Norton DD, Wang X, Kusiak JW (2002). "Aβ 17–42 in Alzheimer's disease activates JNK and caspase‐8 leading to neuronal apoptosis". Brain. 125 (9): 2036–43. doi:10.1093/brain/awf205. PMID 12183349.

Further reading edit

  • Smith JL (2011). "To Go or not to Go, that is the question: Do the N2 and P3 reflect stimulus- or response-related conflict?". International Journal of Psychophysiology. 82 (2): 143–52. doi:10.1016/j.ijpsycho.2011.07.019. PMID 21851842.
  • Wang D, Yang L, Su J, Niu Y, Lei X, Xiong J, Cao X, Hu Y, Mei B, Hu JF (2011). "Attenuation of neurodegenerative phenotypes in Alzheimer-like presenilin 1/presenilin 2 conditional double knockout mice by EUK1001, a promising derivative of xanomeline". Biochemical and Biophysical Research Communications. 410 (2): 229–34. doi:10.1016/j.bbrc.2011.05.120. PMID 21651893.
  • Szczepanik AM, Rampe D, Ringheim GE (2008). "Amyloid-β peptide fragments p3 and p4 induce pro-inflammatory cytokine and chemokine production in vitro and in vivo". Journal of Neurochemistry. 77 (1): 304–17. doi:10.1046/j.1471-4159.2001.00240.x. PMID 11279286. S2CID 84770885.
  • Dickson DW (1997). "The Pathogenesis of Senile Plaques". Journal of Neuropathology & Experimental Neurology. 56 (4): 321–39. doi:10.1097/00005072-199704000-00001. PMID 9100663.

January 19, 2024
peptide, peptide, also, known, amyloid, peptide, peptide, resulting, from, secretase, cleavage, from, amyloid, precursor, protein, known, major, constituent, diffuse, plaques, observed, alzheimer, disease, brains, amyloid, plaques, people, affected, down, synd. p3 peptide also known as amyloid b peptide Ab 17 40 42 is the peptide resulting from the a and g secretase cleavage from the amyloid precursor protein APP It is known to be the major constituent of diffuse plaques observed in Alzheimer s disease AD brains and pre amyloid plaques in people affected by Down syndrome However p3 peptide s role in these diseases is not truly known yet 2 Representation of the 3D structure of p3 peptide 1 This article may be too technical for most readers to understand Please help improve it to make it understandable to non experts without removing the technical details October 2013 Learn how and when to remove this template message Contents 1 Structure 2 Properties 3 Synthesis 4 Role in Alzheimer s disease and Down syndrome 5 References 6 Further readingStructure editThere is little information related to the p3 peptides composition and structure and moreover most of it has to do with characteristics that concern to its role in Alzheimer s disease p3 can be found as a 24 or 26 residues peptide depending on which is gamma secretase s cleavage The peptide which has 26 residues presents the following sequence VFFAEDVGSNKGAIIGLMVGGVVIAT 3 In relation to the secondary structure of p3 peptide it is thought that after the cleavage by the a and g secretases and extraction from the membrane it would convert quickly from the a helix conformation it has when it is part of APPsa sequence to a b hairpin structure Then this highly hydrophobic monomer would rapidly evolve into fibrils with no soluble intermediate forms the ones related to amyloid s structure The main reason why p3 does not aggregate in amyloidogenic forms while Ab does is that the N terminal domain Ab1 16 which is present in Ab s sequence but not in p3 s one is known to protect the hydrophobic core of the oligomers from being dissolved by the watered medium So p3 peptide oligomers would likely expose hydrophobic residues to water and would be less stable As a consequence p3 peptide structural determinants can assemble into fibrils but no oligomeric forms have been identified That is why p3 peptide represents the benign form of amyloid 4 Properties editEnergy plays a very important role in p3 peptides While Ab models have a strong negative energy p3 oligomeric models have a positive one Another characteristic that must be pointed out is that p3 peptides have more solvent exposed hydrophobic surfaces 60 than Ab oligomers do 20 so buried surface areas are not as big within p3 oligomers 30 as they are within Ab oligomers These evidences show that the expected energy of the Ab based oligomeric models of p3 is always positive and that these models expose hydrophobic patches to the solvent and bury a small proportion of their accessible surface within the oligomeric intermediates Having these facts into account we can state that p3 oligomers existence is thermodynamically unfavourable which suggests that the p3 peptide cannot form stable soluble oligomers in the same way Ab does Solution of p3 cannot assemble into stable oligomers as Ab1 42 in the same concentration does Therefore it is very possible that p3 could not last long by itself evolving rapidly into fibrillar forms that hide exposed hydrophobic patches 4 p3 peptides have been analyzed in some researches with Western blot techniques Primary antibodies were used to recognize Ab1 16 residues Unexpectedly it was discovered that the residues did not show any signal This confirms the absence of N terminal domain Ab1 16 in p3 peptides 4 Synthesis editp3 peptide generates from the 17 40 or 17 42 sequence of the amyloid precursor protein APP which is a type I integral membrane protein concerned in neurons synapses in many human tissues Under normal physiological conditions APP is processed with three different proteolytic enzymes a b and g secretases At first APP molecule is cut by a secretase or b secretase and it will produce two different molecules for each case These products are respectively APPsa or a CTFs when cut by a secretase or APPsb and b CTFs when processed by b secretase APPs derivates are sent both to the extra cell while CTFs rest anchored to the plasmatic membrane Then a and b CTFs are processed by g secretase resulting the peptides p3 and Ab respectively and releasing in both cases a cytoplasmic peptide fragment known as the APP intracellular domain AICD Both p3 and Ab are sent to the extracellular medium 4 nbsp APP molecular processing and its different products One of them is p3 peptide which is sent to the extracellular medium 1 Role in Alzheimer s disease and Down syndrome edit nbsp p3 peptide is a product of non amyloidogenic APP processing p3 peptide is known to have a role in AD and DS however it has not been clearly determined yet In order to study the function of p3 peptide in AD specific antibodies location techniques have been used to determine its absence or sparseness in aged non AD brains As it turns out p3 peptide is prevalent in selected areas of AD brain in diffuse deposits and in a subset of dystrophic neuritis both located in the temporal lobe limbic system 5 Although p3 peptide can assemble into fibrillar aggregates its hydrophobic properties make it unable to rest in oligomeric forms This might explain why p3 has no impact on synaptic function and therefore in AD since it is a non amyloidogenic product of APP 4 Despite this fact p3 has been proved to have a role in formation of non fibrillar deposits or lesions associated with DS another neurological disorder that progresses at a faster rate than AD Accordingly DS patients have three copies of the APP gene as they have three copies of the chromosome 21 so APP is overexpressed in the brain and AD develops at an early age The disruption of the normal function of APP in AD and consequently in DS including overexpression or altered processes is the most likely explanation for amyloid plaque formation and subsequent neuronal loss and dementia associated to memory spatial disorientation and deterioration of intellectual capacity 2 Since p3 has not been studied deeply there are different opinions about its role in brain P3 peptides are thought to have a role in neuronal death and in the enhanced inflammatory response in AD and DS as it has been demonstrated that the treatment of cells with the p3 fragment induced by the c Jun N terminal kinases JNK phosphorylation is involved in neuronal cells apoptosis and causes the death of SH SY5Y and IMR 32 human neuroblastoma cells 6 References edit a b PDB 3MOQ a b McCandless Gregory T 2008 Synthesis of disubstituted amino acids and peptide inhibitors of amyloid beta aggregation MS Thesis Louisiana State University OCLC 315888712 Archived from the original on 2013 10 29 Retrieved 2013 10 22 page needed Sequence Search VFFAEDVGSNKGAIIGLMVGGVVIAT Protein Data Bank permanent dead link a b c d e Dulin F Leveille F Ortega JB Mornon JP Buisson A Callebaut I Colloc h N 2008 p3 peptide a truncated form of Ab devoid of synaptotoxic effect does not assemble into soluble oligomers FEBS Letters 582 13 1865 70 doi 10 1016 j febslet 2008 05 002 PMID 18474239 S2CID 43078358 Higgins LS Murphy GM Forno LS Catalano R Cordell B 1996 p3 b Amyloid Peptide Has a Unique and Potentially Pathogenic Immunohistochemical Profile in Alzheimer s Disease Brain The American Journal of Pathology 149 2 585 96 PMC 1865300 PMID 8701997 Wei W Norton DD Wang X Kusiak JW 2002 Ab 17 42 in Alzheimer s disease activates JNK and caspase 8 leading to neuronal apoptosis Brain 125 9 2036 43 doi 10 1093 brain awf205 PMID 12183349 Further reading editSmith JL 2011 To Go or not to Go that is the question Do the N2 and P3 reflect stimulus or response related conflict International Journal of Psychophysiology 82 2 143 52 doi 10 1016 j ijpsycho 2011 07 019 PMID 21851842 Wang D Yang L Su J Niu Y Lei X Xiong J Cao X Hu Y Mei B Hu JF 2011 Attenuation of neurodegenerative phenotypes in Alzheimer like presenilin 1 presenilin 2 conditional double knockout mice by EUK1001 a promising derivative of xanomeline Biochemical and Biophysical Research Communications 410 2 229 34 doi 10 1016 j bbrc 2011 05 120 PMID 21651893 Szczepanik AM Rampe D Ringheim GE 2008 Amyloid b peptide fragments p3 and p4 induce pro inflammatory cytokine and chemokine production in vitro and in vivo Journal of Neurochemistry 77 1 304 17 doi 10 1046 j 1471 4159 2001 00240 x PMID 11279286 S2CID 84770885 Dickson DW 1997 The Pathogenesis of Senile Plaques Journal of Neuropathology amp Experimental Neurology 56 4 321 39 doi 10 1097 00005072 199704000 00001 PMID 9100663 Retrieved from https en wikipedia org w index php title P3 peptide amp oldid 1174984655, wikipedia, wiki, book, books, library,

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