Periodontal fiber
Periodontal ligament | |
---|---|
Details | |
Precursor | dental follicle |
Identifiers | |
Latin | fibra periodontalis |
Acronym(s) | PDL |
MeSH | D010513 |
FMA | 56665 |
Anatomical terminology |
The periodontal ligament, commonly abbreviated as the PDL, is a group of specialized connective tissue fibers that essentially attach a tooth to the alveolar bone within which it sits.[1] It inserts into root cementum one side and onto alveolar bone on the other.
Structure
The PDL consists of principal fibres, loose connective tissue, blast and clast cells, oxytalan fibres and Cell Rest of Malassez.[2]
Alveolodental ligament
The main principal fiber group is the alveolodental ligament, which consists of five fiber subgroups: alveolar crest, horizontal, oblique, apical, and interradicular on multirooted teeth. Principal fibers other than the alveolodental ligament are the transseptal fibers.
All these fibers help the tooth withstand the naturally substantial compressive forces that occur during chewing and remain embedded in the bone. The ends of the principal fibers that are within either cementum or alveolar bone proper are considered Sharpey fibers.
- Alveolar crest fibers (I) run from the cervical part of the root to the alveolar bone crest
- Horizontal fibers (J) attach to the cementum apical to the alveolar crest fibers and run perpendicularly from the root of the tooth to the alveolar bone..
- Oblique fibers (K) are the most numerous fibers in the periodontal ligament, running from cementum in an oblique direction to insert into bone coronally. These fibres resist vertical & intrusive forces
- Apical fibers are found radiating from cementum around the apex of the root to the bone, forming base of the socket or alveolus.
- Interradicular fibers are only found between the roots of multirooted teeth, such as premolars and molars. They extend from radicular cementum to interradicular alveolar bone.
Transseptal fibers
Transseptal fibers (H) extend interproximally over the alveolar bone crest and are embedded in the cementum of adjacent teeth; they form an interdental ligament. These fibers keep all the teeth aligned. These fibers may be considered as belonging to the gingival tissue because they do not have an osseous attachment.[3].These fibres are consistent and are reconstructed even after the destruction of alveolar bone.
Loose connective tissue
Loose connective tissue contains fibres, extracellular matrix, cells, nerves and blood vessels. The extracellular compartment consists of Type 1, 3, and 5 collagen fibers bundles embedded in intercellular substance. The PDL collagen fibers are categorized according to their orientation and location along the tooth. The cells include fibroblast, defence cells and undifferentiated mesenchymal cells.
Cell Rest of Malassez
These groups of epithelial cells become located in the mature PDL after the disintegration of Hertwig epithelial root sheath during the formation of the root.[2] They form a plexus that surrounds the tooth. Cell Rests of Malassez might proliferate during inflammation which may lead to radicular cyst formation in later life.
Oxytalan fibres
Oxytalan fibres are unique to the PDL and are elastic in nature. It inserts into cementum and runs in 2 directions; parallel to root surface and oblique to root surface. The function is thought to maintain the patency of blood vessels during occlusal loading. Further research is needed to determine the function of oxytalan fibres.[4]
Composition
The PDL substance has been estimated to be 70% water, which is thought to have a significant effect on the tooth's ability to withstand stress loads. The completeness and vitality of the PDL are essential for the functioning of the tooth.
The PDL ranges in width from 0.15 to 0.38mm with its thinnest part located in the middle third of the root.[5] The width progressively decreases with age.
The PDL is a part of the periodontium that provides for the attachment of the teeth to the surrounding alveolar bone by way of the cementum.
The PDL appears as the periodontal space of 0.4 to 1.5 mm on radiographs, a radiolucent area between the radiopaque lamina dura of the alveolar bone proper and the radiopaque cementum.
Development
PDL cells are one of the many cells derived from the dental follicle and this occurs after crown formation is completed and when the roots start developing. These cells will remodel the dental follicle to form the PDL.[5] Formation of PDL will start at the cementoenamel junction and proceeds in an apical direction.[6]
Effects of mechanical forces
Movement of teeth is determined by two factors: deposition of bone on the tension side and resorption of the bone on the compression side of the periodontal ligament (PDL). During this movement, bone remodelling is initiated by the PDL in which forces are transmitted from the tooth to the alveolar bone. Fibroblasts of the PDL will react to mechanical stress, therefore affecting osteoblastogenesis and osteoclastogenesis of the cells. When mechanical stimuli are introduced to the cells osteocytes in the PDL will differentiate into osteoclasts which will then reform and remodel the bone structure in the affected area. For example, orthodontic treatment involves application of a mechanical force on to the teeth to align them and this is done through this complex combination of physical and cellular processes.[7]
Function
Functions of PDL are supportive, sensory, nutritive, and remodelling.[8]
Support
The PDL is a part of the periodontium that provides for the attachment of the teeth to the surrounding alveolar bone by way of the cementum. PDL fibres also provide a role in load transfer between the teeth and alveolar bone. (PDL fibres absorb and transmit forces between teeth and alveolar bone. It acts as an effective support during the masticatory function.)[9]
Sensory
PDL is heavily innervated; it involves mechanoreception, nociception and reflexes. Periodontal mechanoreceptors are present in PDL. They will transmit information about the stimulated tooth, direction and amplitude of forces.[10]
Nutritive
It maintains the vitality of the surrounding cells. (PDL is heavily anastomosed). There are three principal sources of blood vessels which are apical vessels, perforating vessels and gingival vessels. Apical vessels originate from vessels that supply the pulp. Perforating vessels originate from lamina dura and the vessels perforate the socket wall (cribriform plate). Gingival vessels are derived from the gingival tissue. Outer layers of blood supply in PDL may help in mechanical suspension and support of the tooth while inner layers of blood vessels supply surrounding PDL tissues.[11]
Remodeling
There are progenitor cells in the periodontal ligament that can differentiate into osteoblasts for the physiological maintenance of alveolar bone and, most likely, for its repair as well.
Clinical significance
Injury
- When traumatic forces of occlusion are placed on a tooth, the PDL widens to take the extra forces. Thus, early occlusal trauma can be viewed on radiographs as a widening of the periodontal ligament space. Thickening of the lamina dura in response is also possible. Clinically, occlusal trauma is noted by the late manifestation of increased mobility of the tooth and possibly the presence of pathological tooth migration.[5]
- Damage to the PDL may result in tooth ankylosis to the jawbone, making the tooth lose its continuous eruption ability. Dental trauma, such as subluxation, may cause tearing of the PDL and pain during function (eating).[12]
- The PDL cells of an avulsed tooth is at risk of drying and desiccation if left in dry storage. Wet storage in an isotonic liquid, although a superior method to dry storage, can preserve PDL vitality depending on the medium but not for an indefinite period of time. All of these can lead to loss of vitality of the PDL and depending on the duration of storage, this can affect the success of subsequent replantation.[13]
Disease
- The epithelial rests of Malassez can become cystic, usually forming nondiagnostic, radiolucent apical lesions that can be seen on radiographs. This occurs as a result of chronic periapical inflammation after pulpitis occurs and must be surgically removed.[5]
- The PDL also undergoes drastic changes with chronic periodontal disease that involves the deeper structures of the periodontium with periodontitis. The fibers of the PDL become disorganized, and their attachments to either the alveolar bone proper or cementum through Sharpey fibers are lost because of the resorption of these two hard dental tissue.[5]
- Pathological damaged or diseased PDL can result in delayed healing of the alveolar socket in cases where the diseased tooth is ultimately extracted.[14]
Effect of tobacco smoking and nicotine
There is a relationship between smoking tobacco and periodontal disease, wound healing and oral cancers.[15]
Nicotine, the major pharmacologically active ingredient in tobacco smoke, lessens a host's ability to defend against bacterial invasion induced by plaque. It is also the ingredient responsible for addiction.[16]
Tobacco smoking impairs phagocytic and chemotactic activities of leukocytes[17] and impedes wound healing,[18] specifically by affecting gingival blood flow.[19][20]
Cigarette smokers are more likely to experience destruction of the alveolar bone and periodontal ligament and are at a higher risk of developing periodontal disease.[21][22]
Nicotine and lipopolysaccharides synergistically induce the production of nitric oxide (NO) and PGE2, and increase inducible nitric oxide synthase (iNOS) and COX-2 expression in human periodontal ligament (hPDL) cells.
At the cellular level, nicotine reduces the proliferation of red blood cells, macrophages, and fibroblasts and increases platelet adhesiveness.
Macroscopically, this affects healing and tissue perfusion due to micro clot formation in the blood vessels.[23][24] Nicotine also has a sympathomimetic action, stimulating epinephrine and norepinephrine release, which causes vasoconstriction and limits tissue perfusion. Nicotine jeopardises bone formation by inhibiting neovascularization and osteoblastic differentiation.[25][26][27][28][29]
Ankylosis
Ankylosis is a condition where the cementum of the tooth's root fuses with the bone that is around the tooth. The osseous tissue replaces the periodontal ligament which causes the tooth to be fixed and cannot undergo eruptive change. Ankylosis usually occurs in primary molars, however this can also take place in other primary teeth, as well as secondary dentition. Ankylosis is common in the anterior tooth after trauma and can be referred to as replacement resorption. In this process PDL cells are destroyed and as a result the cells of the alveolar bone will perform most of the healing. Radiographic examination of a patient with ankylosis may also reveal a loss of the PDL and bony bridging.
Effect of nutrition
Nutritional status of an individual can be a crucial factor in the progression and healing of periodontal tissues. The relationship between oral health and systemic health has become an increasingly important subject. Studies have suggested that vitamins D and C in particular have a certain grade of relationship with periodontal health. However, it is important to note that supplementation of vitamins is not enough to reverse the periodontium to a healthy state and that further research is needed to confirm theories.
For example, scurvy is a disease resulting from a severe deficiency of vitamin C (ascorbic acid). Vitamin C is essential for the synthesis of collagen fibers. collagen synthesis.
See also
References
- ↑ Wolf HF, Rateitschak KH (2005). Periodontology. Thieme. pp. 12–. ISBN 978-0-86577-902-0. Retrieved June 21, 2011.
- ↑ Listgarten MA. ". Principal fibers of the periodontal ligament". University of Pennsylvania and Temple University. Archived from the original on June 20, 2012.
It is the different composition of collagens which give various ECM functions and abilities. There is a mixture of thick and thin fibres in the PDL. It is important to note that, in reality, the fibres are not as defined as these classifications.
- ↑ Naci A (2013). Ten Cate's Oral Histology. Elsevier. p. 274. ISBN 978-0-323-07846-7.
- ↑ Strydom H, Maltha JC, Kuijpers-Jagtman AM, Von den Hoff JW (August 2012). "The oxytalan fibre network in the periodontium and its possible mechanical function". Archives of Oral Biology. 57 (8): 1003–11. doi:10.1016/j.archoralbio.2012.06.003. PMID 22784380.
- 1 2 3 4 Yao S, Pan F, Prpic V, Wise GE (August 2008). "Differentiation of stem cells in the dental follicle". Journal of Dental Research. 87 (8): 767–71. doi:10.1177/154405910808700801. PMC 2553250. PMID 18650550.
- ↑ de Jong T, Bakker AD, Everts V, Smit TH (December 2017). "The intricate anatomy of the periodontal ligament and its development: Lessons for periodontal regeneration". Journal of Periodontal Research. 52 (6): 965–974. doi:10.1111/jre.12477. PMID 28635007. S2CID 38159994.
- ↑ Li M, Zhang C, Yang Y (January 2019). "Effects of mechanical forces on osteogenesis and osteoclastogenesis in human periodontal ligament fibroblasts: A systematic review of in vitro studies". Bone & Joint Research. 8 (1): 19–31. doi:10.1302/2046-3758.81.BJR-2018-0060.R1. PMC 6359886. PMID 30800296.
- ↑ Listgarten MA. "Periodontal ligament". University of Pennsylvania and Temple University. Archived from the original on June 16, 2010.
- ↑ McCormack SW, Witzel U, Watson PJ, Fagan MJ, Gröning F (2014). "The biomechanical function of periodontal ligament fibres in orthodontic tooth movement". PLOS ONE. 9 (7): e102387. Bibcode:2014PLoSO...9j2387M. doi:10.1371/journal.pone.0102387. PMC 4103804. PMID 25036099.
- ↑ Trulsson M (April 2006). "Sensory-motor function of human periodontal mechanoreceptors". Journal of Oral Rehabilitation. 33 (4): 262–73. doi:10.1111/j.1365-2842.2006.01629.x. PMID 16629881.
- ↑ Institute of Anatomy, University of Veterinary Medicine Hannover, Bischofsholer Damm 15, D-30173 Hannover, Germany
- ↑ Zadik Y (December 2008). "Algorithm of first-aid management of dental trauma for medics and corpsmen". Dental Traumatology. 24 (6): 698–701. doi:10.1111/j.1600-9657.2008.00649.x. PMID 19021668.
- ↑ Layug ML, Barrett EJ, Kenny DJ (May 1998). "Interim storage of avulsed permanent teeth". Journal. 64 (5): 357–63, 365–9. PMID 9648418.
- ↑ Kim JH, Koo KT, Capetillo J, Kim JJ, Yoo JM, Ben Amara H, et al. (June 2017). "Periodontal and endodontic pathology delays extraction socket healing in a canine model". Journal of Periodontal & Implant Science. 47 (3): 143–153. doi:10.5051/jpis.2017.47.3.143. PMC 5494309. PMID 28680710.
- ↑ World Health Organisation Monograph on Tobacco Cessation and Oral Health Integration, Geneva (2017)
- ↑ Whiteford L (December 2003). "Nicotine, CO and HCN: the detrimental effects of smoking on wound healing". British Journal of Community Nursing. 8 (12): S22-6. doi:10.12968/bjcn.2003.8.sup6.12554. PMID 14700008.
- ↑ Tomar SL, Asma S (May 2000). "Smoking-attributable periodontitis in the United States: findings from NHANES III. National Health and Nutrition Examination Survey". Journal of Periodontology. 71 (5): 743–51. doi:10.1902/jop.2000.71.5.743. PMID 10872955.
- ↑ Genco RJ, Borgnakke WS (June 2013). "Risk factors for periodontal disease". Periodontology 2000. 62 (1): 59–94. doi:10.1111/j.1600-0757.2012.00457.x. PMID 23574464.
- ↑ Leite FR, Nascimento GG, Scheutz F, López R (June 2018). "Effect of Smoking on Periodontitis: A Systematic Review and Meta-regression". American Journal of Preventive Medicine. 54 (6): 831–841. doi:10.1016/j.amepre.2018.02.014. PMID 29656920.
- ↑ Qandil R, Sandhu HS, Matthews DC (March 1997). "Tobacco smoking and periodontal diseases". Journal (Canadian Dental Association). 63 (3): 187–92, 194–5. PMID 9086680.
- ↑ Morozumi T, Kubota T, Sato T, Okuda K, Yoshie H (April 2004). "Smoking cessation increases gingival blood flow and gingival crevicular fluid". Journal of Clinical Periodontology. 31 (4): 267–72. doi:10.1111/j.1600-051x.2004.00476.x. PMID 15016254.
- ↑ Johnson GK, Todd GL, Johnson WT, Fung YK, Dubois LM (May 1991). "Effects of topical and systemic nicotine on gingival blood flow in dogs". Journal of Dental Research. 70 (5): 906–9. doi:10.1177/00220345910700050801. PMID 2022772. S2CID 28627546.
- ↑ Ciftçi O, Günday M, Calişkan M, Güllü H, Güven A, Müderrisoğlu H (June 2013). "Light cigarette smoking and vascular function". Acta Cardiologica. 68 (3): 255–61. doi:10.1080/ac.68.3.2983419. PMID 23882870. S2CID 42726406.
- ↑ Tomar SL, Asma S (May 2000). "Smoking-attributable periodontitis in the United States: findings from NHANES III. National Health and Nutrition Examination Survey". Journal of Periodontology. 71 (5): 743–51. doi:10.1902/jop.2000.71.5.743. PMID 10872955.
- ↑ Pi SH, Jeong GS, Oh HW, Kim YS, Pae HO, Chung HT, et al. (April 2010). "Heme oxygenase-1 mediates nicotine- and lipopolysaccharide-induced expression of cyclooxygenase-2 and inducible nitric oxide synthase in human periodontal ligament cells". Journal of Periodontal Research. 45 (2): 177–83. doi:10.1111/j.1600-0765.2009.01215.x. PMID 20470258.
- ↑ Jones JK, Triplett RG (March 1992). "The relationship of cigarette smoking to impaired intraoral wound healing: a review of evidence and implications for patient care". Journal of Oral and Maxillofacial Surgery. 50 (3): 237–9, discussion 239–40. doi:10.1016/0278-2391(92)90318-t. PMID 1542066.
- ↑ Saito Y, Sato S, Oginuma T, Saito Y, Arai Y, Ito K (May 2013). "Effects of nicotine on guided bone augmentation in rat calvarium". Clinical Oral Implants Research. 24 (5): 531–5. doi:10.1111/j.1600-0501.2011.02416.x. PMID 22276738.
- ↑ Donigan JA, Fredericks DC, Nepola JV, Smucker JD (December 2012). "The effect of transdermal nicotine on fracture healing in a rabbit model". Journal of Orthopaedic Trauma. 26 (12): 724–7. doi:10.1097/bot.0b013e318270466f. PMID 22955337. S2CID 29873064.
- ↑ Glowacki J, Schulten AJ, Perrott D, Kaban LB (February 2008). "Nicotine impairs distraction osteogenesis in the rat mandible". International Journal of Oral and Maxillofacial Surgery. 37 (2): 156–61. doi:10.1016/j.ijom.2007.08.001. PMID 17983728.
External links
- Nanci A, Bosshardt DD (2006). "Structure of periodontal tissues in health and disease". Periodontology 2000. 40: 11–28. doi:10.1111/j.1600-0757.2005.00141.x. PMID 16398683.