M protein (Streptococcus): Difference between revisions
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{{Infobox protein family |
{{Infobox protein family |
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| Symbol = Gram_pos_anchor |
| Symbol = Gram_pos_anchor |
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| ⚫ | '''M protein''' is a [[virulence factor]] that can be produced by certain species of ''[[Streptococcus]]''.<ref name="pmid10846214">{{cite journal |vauthors=Chanter N, Talbot NC, Newton JR, Hewson D, Verheyen K |title=Streptococcus equi with truncated M-proteins isolated from outwardly healthy horses |journal=Microbiology |issue= Pt 6 |pages=1361–9 |volume=146 |date=June 2000 |pmid=10846214 |doi= 10.1099/00221287-146-6-1361|url=http://mic.sgmjournals.org/cgi/pmidlookup?view=long&pmid=10846214|doi-access=free }}</ref> |
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| ⚫ | '''M protein''' is a [[virulence factor]] that can be produced by certain species of ''[[Streptococcus]]''.<ref name="pmid10846214">{{cite journal | |
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Viruses, [[parasite]]s and [[Zinc dependent phospholipase C|bacteria]] are covered in [[protein]] and [[sugar]] [[molecule]]s that help them gain entry into a host by counteracting the host's |
Viruses, [[parasite]]s and [[Zinc dependent phospholipase C|bacteria]] are covered in [[protein]] and [[sugar]] [[molecule]]s that help them gain entry into a host by counteracting the host's defenses. One such molecule is the M protein produced by certain streptococcal [[bacterium|bacteria]]. At its C-terminus within the cell wall, M [[protein]]s embody a [[protein motif|motif]] that is now known to be shared by many [[Gram-positive]] [[bacteria]]l surface [[proteins]]. The [[sequence motif|motif]] includes a [[conserved sequence|conserved]] hexapeptide LPXTGE, which precedes a [[hydrophobic]] C-terminal [[Cell membrane|membrane]] spanning domain, which itself precedes a cluster of [[Base (chemistry)|basic]] [[residue (chemistry)|residues]] at the C-terminus.<ref name="pmid2188957">{{cite journal |vauthors=Schneewind O, Jones KF, Fischetti VA | title = Sequence and structural characteristics of the trypsin-resistant T6 surface protein of group A streptococci | journal = J. Bacteriol. | volume = 172 | issue = 6 | pages = 3310–7 |date=June 1990 | doi = 10.1128/jb.172.6.3310-3317.1990 | pmid = 2188957 | pmc = 209141 }}</ref><ref name="pmid2287281">{{cite journal |vauthors=Fischetti VA, Pancholi V, Schneewind O | title = Conservation of a hexapeptide sequence in the anchor region of surface proteins from gram-positive cocci | journal = Mol. Microbiol. | volume = 4 | issue = 9 | pages = 1603–5 |date=September 1990 | pmid = 2287281 | doi = 10.1111/j.1365-2958.1990.tb02072.x}}</ref> |
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M protein is strongly anti-phagocytic and is |
M protein is strongly anti-phagocytic and is the major virulence factor for group A streptococci (''Streptococcus pyogenes''). It binds to serum [[factor H]], destroying [[C3-convertase]] and preventing [[opsonization]] by [[C3b]]. However plasma B cells can generate antibodies against M protein which will help in opsonization and further the destruction of the microorganism by the macrophages and neutrophils. [[Cross-reactivity]] of anti-M protein antibodies with heart muscle has been suggested to be associated in some way with [[rheumatic fever]]. |
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It was originally identified by [[Rebecca Lancefield]],<ref name="urlStreptococcal M protein: molecular design and biological behavior. |
It was originally identified by [[Rebecca Lancefield]],<ref name="urlStreptococcal M protein: molecular design and biological behavior.">{{cite web |url=http://cmr.asm.org/cgi/content/abstract/2/3/285 |title=Streptococcal M protein: molecular design and biological behavior. |access-date=2009-06-21}}</ref> who also formulated the [[Lancefield grouping|Lancefield classification system]] for streptococcal bacteria. Bacteria like ''S. pyogenes,'' which possess M protein are classified in group A of the Lancefield system. |
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== Therapeutic approaches == |
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In recent years, the emergence of antibiotic resistance among streptococcal bacteria, particularly [[Streptococcus pyogenes|Group A Streptococcus (GAS)]] or Streptococcus pyogenes, has posed significant challenges to traditional therapeutic approaches.<ref name="Carapetis-2005">{{Cite journal |last1=Carapetis |first1=Jonathan R. |last2=Steer |first2=Andrew C. |last3=Mulholland |first3=E. Kim |last4=Weber |first4=Martin |date=November 2005 |title=The global burden of group A streptococcal diseases |url=https://pubmed.ncbi.nlm.nih.gov/16253886/ |journal=The Lancet. Infectious Diseases |volume=5 |issue=11 |pages=685–694 |doi=10.1016/S1473-3099(05)70267-X |issn=1473-3099 |pmid=16253886}}</ref> The M protein, as a major virulence factor of GAS, has been a focal point for developing novel therapeutic strategies aimed at combating streptococcal infections. |
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Current therapeutic approaches targeting M protein predominantly involve [[Antibiotic|antibiotics]] and immunomodulatory agents. Antibiotics such as [[penicillin]] and [[amoxicillin]] have been the mainstay of treatment for streptococcal infections.<ref name="Carapetis-2005" /> However, the rise of antibiotic-resistant strains underscores the urgent need for alternative therapies. In this context, immunomodulatory agents, including [[Immunoglobulin therapy|intravenous immunoglobulin (IVIG)]], have shown promise in [[Mitigation|mitigating]] the inflammatory response associated with severe GAS infections, although their efficacy in targeting M protein specifically remains to be fully elucidated. |
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== Development of vaccines == |
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The development of [[Vaccine|vaccines]] targeting M protein or its associated [[Epitope|epitopes]] represents a promising avenue for the prevention and treatment of streptococcal infections. Vaccines designed to induce protective immune responses against M protein have the potential to confer long-term immunity and reduce the incidence of GAS-related diseases, including [[pharyngitis]], [[impetigo]], and invasive infections such as [[necrotizing fasciitis]] and [[Toxic shock syndrome|streptococcal toxic shock syndrome]].<ref name="Dale-2013">{{Cite journal |last1=Dale |first1=James B. |last2=Fischetti |first2=Vincent A. |last3=Carapetis |first3=Jonathan R. |last4=Steer |first4=Andrew C. |last5=Sow |first5=Samba |last6=Kumar |first6=Rajesh |last7=Mayosi |first7=Bongani M. |last8=Rubin |first8=Fran A. |last9=Mulholland |first9=Kim |last10=Hombach |first10=Joachim Maria |last11=Schödel |first11=Florian |last12=Henao-Restrepo |first12=Ana Maria |date=2013-04-18 |title=Group A streptococcal vaccines: paving a path for accelerated development |url=https://pubmed.ncbi.nlm.nih.gov/23598485/ |journal=Vaccine |volume=31 |issue=Suppl 2 |pages=B216–222 |doi=10.1016/j.vaccine.2012.09.045 |issn=1873-2518 |pmid=23598485}}</ref> |
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Several vaccine candidates targeting M protein have been explored in [[Preclinical development|preclinical]] and [[Clinical trial|clinical studies]].<ref name="Dale-2013" /> These vaccines aim to elicit [[Antibody|antibodies]] that recognize and neutralize M protein, thereby preventing bacterial attachment and invasion. Furthermore, efforts have been made to enhance vaccine efficacy by incorporating conserved epitopes of M protein or employing novel adjuvants to boost immune responses. |
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One promising approach involves the use of multi-epitope vaccines that target multiple [[Antigen|antigenic]] sites on M protein, thereby reducing the likelihood of [[Immune system|immune]] evasion by GAS strains expressing variant M protein [[Protein isoform|isoforms]].<ref name="Dale-2013" /> Additionally, advances in vaccine delivery systems, such as nanoparticle-based platforms and [[Mucosal immunology|mucosal]] vaccination routes, hold potential for enhancing vaccine immunogenicity and efficacy against streptococcal infections. |
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Despite these advancements, several challenges remain in the development and implementation of M protein-based vaccines. These include the identification of highly conserved epitopes capable of eliciting protective [[Immune response|immune responses]] across diverse GAS strains, as well as addressing potential [[autoimmunity]] associated with molecular mimicry between M protein and host tissues, particularly in the context of [[rheumatic fever]]. |
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== Future perspectives == |
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Targeting M protein represents a promising approach for the development of novel therapeutics and vaccines against streptococcal infections. By leveraging advances in immunology, vaccinology, and molecular biology, researchers are poised to overcome existing challenges and realize the potential of M protein-based interventions in combating this significant public health threat. |
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==Literature== |
==Literature== |
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* {{cite journal | |
* {{cite journal |vauthors=Fischetti VA, Pancholi V, Schneewind O | title = Conservation of a hexapeptide sequence in the anchor region of surface proteins from gram-positive cocci | journal = Mol. Microbiol. | volume = 4 | issue = 9 | pages = 1603–5 |date=September 1990 | pmid = 2287281 | doi = 10.1111/j.1365-2958.1990.tb02072.x}} |
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* {{Cite journal |
* {{Cite journal |
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|author1=Pierre R. Smeesters |author2=David J. McMillan |author3=Kadaba S. Sriprakash | title = The streptococcal M protein: a highly versatile molecule |
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| ⚫ | |||
| title = The streptococcal M protein: a highly versatile molecule |
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| ⚫ | |||
| volume = 18 |
| volume = 18 |
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| issue = 6 |
| issue = 6 |
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| pages = 275–282 |
| pages = 275–282 |
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|date=June 2010 |
|date=June 2010 |
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| doi = 10.1016/j.tim.2010.02.007 |
| doi = 10.1016/j.tim.2010.02.007 |
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| pmid = 20347595 |
| pmid = 20347595 |
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}} |
}} |
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==References== |
==References== |
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{{reflist}} |
{{reflist}} |
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[[Category:Virulence factors]] |
[[Category:Virulence factors]] |
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[[Category:Streptococcal proteins]] |
[[Category:Streptococcal proteins]] |
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{{medicine-stub}} |
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Latest revision as of 04:36, 11 May 2024
| Gram_pos_anchor | |||||||||
|---|---|---|---|---|---|---|---|---|---|
| Identifiers | |||||||||
| Symbol | Gram_pos_anchor | ||||||||
| Pfam | PF00746 | ||||||||
| Pfam clan | CL0501 | ||||||||
| InterPro | IPR019948 | ||||||||
| PROSITE | PDOC00373 | ||||||||
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M protein is a virulence factor that can be produced by certain species of Streptococcus.[1]
Viruses, parasites and bacteria are covered in protein and sugar molecules that help them gain entry into a host by counteracting the host's defenses. One such molecule is the M protein produced by certain streptococcal bacteria. At its C-terminus within the cell wall, M proteins embody a motif that is now known to be shared by many Gram-positive bacterial surface proteins. The motif includes a conserved hexapeptide LPXTGE, which precedes a hydrophobic C-terminal membrane spanning domain, which itself precedes a cluster of basic residues at the C-terminus.[2][3]
M protein is strongly anti-phagocytic and is the major virulence factor for group A streptococci (Streptococcus pyogenes). It binds to serum factor H, destroying C3-convertase and preventing opsonization by C3b. However plasma B cells can generate antibodies against M protein which will help in opsonization and further the destruction of the microorganism by the macrophages and neutrophils. Cross-reactivity of anti-M protein antibodies with heart muscle has been suggested to be associated in some way with rheumatic fever.
It was originally identified by Rebecca Lancefield,[4] who also formulated the Lancefield classification system for streptococcal bacteria. Bacteria like S. pyogenes, which possess M protein are classified in group A of the Lancefield system.
Therapeutic approaches
[edit]In recent years, the emergence of antibiotic resistance among streptococcal bacteria, particularly Group A Streptococcus (GAS) or Streptococcus pyogenes, has posed significant challenges to traditional therapeutic approaches.[5] The M protein, as a major virulence factor of GAS, has been a focal point for developing novel therapeutic strategies aimed at combating streptococcal infections.
Current therapeutic approaches targeting M protein predominantly involve antibiotics and immunomodulatory agents. Antibiotics such as penicillin and amoxicillin have been the mainstay of treatment for streptococcal infections.[5] However, the rise of antibiotic-resistant strains underscores the urgent need for alternative therapies. In this context, immunomodulatory agents, including intravenous immunoglobulin (IVIG), have shown promise in mitigating the inflammatory response associated with severe GAS infections, although their efficacy in targeting M protein specifically remains to be fully elucidated.
Development of vaccines
[edit]The development of vaccines targeting M protein or its associated epitopes represents a promising avenue for the prevention and treatment of streptococcal infections. Vaccines designed to induce protective immune responses against M protein have the potential to confer long-term immunity and reduce the incidence of GAS-related diseases, including pharyngitis, impetigo, and invasive infections such as necrotizing fasciitis and streptococcal toxic shock syndrome.[6]
Several vaccine candidates targeting M protein have been explored in preclinical and clinical studies.[6] These vaccines aim to elicit antibodies that recognize and neutralize M protein, thereby preventing bacterial attachment and invasion. Furthermore, efforts have been made to enhance vaccine efficacy by incorporating conserved epitopes of M protein or employing novel adjuvants to boost immune responses.
One promising approach involves the use of multi-epitope vaccines that target multiple antigenic sites on M protein, thereby reducing the likelihood of immune evasion by GAS strains expressing variant M protein isoforms.[6] Additionally, advances in vaccine delivery systems, such as nanoparticle-based platforms and mucosal vaccination routes, hold potential for enhancing vaccine immunogenicity and efficacy against streptococcal infections.
Despite these advancements, several challenges remain in the development and implementation of M protein-based vaccines. These include the identification of highly conserved epitopes capable of eliciting protective immune responses across diverse GAS strains, as well as addressing potential autoimmunity associated with molecular mimicry between M protein and host tissues, particularly in the context of rheumatic fever.
Future perspectives
[edit]Targeting M protein represents a promising approach for the development of novel therapeutics and vaccines against streptococcal infections. By leveraging advances in immunology, vaccinology, and molecular biology, researchers are poised to overcome existing challenges and realize the potential of M protein-based interventions in combating this significant public health threat.
Literature
[edit]- Fischetti VA, Pancholi V, Schneewind O (September 1990). "Conservation of a hexapeptide sequence in the anchor region of surface proteins from gram-positive cocci". Mol. Microbiol. 4 (9): 1603–5. doi:10.1111/j.1365-2958.1990.tb02072.x. PMID 2287281.
- Pierre R. Smeesters; David J. McMillan; Kadaba S. Sriprakash (June 2010). "The streptococcal M protein: a highly versatile molecule". Trends in Microbiology. 18 (6): 275–282. doi:10.1016/j.tim.2010.02.007. PMID 20347595.
References
[edit]- ^ Chanter N, Talbot NC, Newton JR, Hewson D, Verheyen K (June 2000). "Streptococcus equi with truncated M-proteins isolated from outwardly healthy horses". Microbiology. 146 (Pt 6): 1361–9. doi:10.1099/00221287-146-6-1361. PMID 10846214.
- ^ Schneewind O, Jones KF, Fischetti VA (June 1990). "Sequence and structural characteristics of the trypsin-resistant T6 surface protein of group A streptococci". J. Bacteriol. 172 (6): 3310–7. doi:10.1128/jb.172.6.3310-3317.1990. PMC 209141. PMID 2188957.
- ^ Fischetti VA, Pancholi V, Schneewind O (September 1990). "Conservation of a hexapeptide sequence in the anchor region of surface proteins from gram-positive cocci". Mol. Microbiol. 4 (9): 1603–5. doi:10.1111/j.1365-2958.1990.tb02072.x. PMID 2287281.
- ^ "Streptococcal M protein: molecular design and biological behavior". Retrieved 2009-06-21.
- ^ a b Carapetis, Jonathan R.; Steer, Andrew C.; Mulholland, E. Kim; Weber, Martin (November 2005). "The global burden of group A streptococcal diseases". The Lancet. Infectious Diseases. 5 (11): 685–694. doi:10.1016/S1473-3099(05)70267-X. ISSN 1473-3099. PMID 16253886.
- ^ a b c Dale, James B.; Fischetti, Vincent A.; Carapetis, Jonathan R.; Steer, Andrew C.; Sow, Samba; Kumar, Rajesh; Mayosi, Bongani M.; Rubin, Fran A.; Mulholland, Kim; Hombach, Joachim Maria; Schödel, Florian; Henao-Restrepo, Ana Maria (2013-04-18). "Group A streptococcal vaccines: paving a path for accelerated development". Vaccine. 31 (Suppl 2): B216–222. doi:10.1016/j.vaccine.2012.09.045. ISSN 1873-2518. PMID 23598485.