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Inicio Revista Clínica de Periodoncia, Implantología y Rehabilitación Oral Variabilidad de la Síntesis de RANKL por Linfocitos T frente a Distintos Seroti...
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Vol. 3. Núm. 1.
Páginas 19-23 (abril 2010)
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Vol. 3. Núm. 1.
Páginas 19-23 (abril 2010)
Open Access
Variabilidad de la Síntesis de RANKL por Linfocitos T frente a Distintos Serotipos Capsulares de Porphyromonas gingivalis
Variability in the RANKL Synthesis by T Lymphocytes in Response to Different Porphyromonas gingivalis Capsular Serotypes
Visitas
1744
M. Navarrete1, A. Silva2, M. Sanz3, R. Vernal1,
Autor para correspondencia
rvernal@uchile.cl

Correspondencia autor: Laboratorio de Biología Periodontal, Facultad de Odontología, Universidad de Chile. Sergio Livingstone 943, Independencia, Santiago, Chile. Fono: 56-2-9781815 / Fax: 56-2-9781833.
1 Laboratorio de Biología Periodontal, Departamento de Odontología Conservadora, Facultad de Odontología, Universidad de Chile, Santiago, Chile
2 Departamento de Medicina Celular y Molecular, Centro de Investigaciones Biológicas, Consejo Superior de Investigaciones Cientí cas (CSIC), Madrid, España
3 Departamento de Estomatología III, Facultad de Odontología, Universidad Complutense de Madrid, Madrid, España
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Información del artículo
Resumen
Propósito

Las periodontitis representan un grupo heterogéneo de infecciones periodontales cuya etiología son las bacterias residentes en el bio lm subgingival. Aunque este bio lm está constituido por una amplia variedad de especies bacterianas, sólo un número limitado de especies, como Porphyromonas gingivalis, se ha asociado a la etiología de la enfermedad. P. gingivalis expresa diversos factores de virulencia que pueden causar daño directo a los tejidos del hospedero; sin embargo, su mayor patogenicidad involucra la inducción de una respuesta inmuno-inflamatoria, durante la cual se secretan una amplia variedad de citoquinas, quimioquinas y mediadores inflamatorios que pueden inducir la destrucción de los tejidos de soporte de los dientes y la pérdida de ellos.

Método

En esta investigación, se evaluó si los distintos serotipos capsulares (K) de P. gingivalis pueden determinar los niveles de síntesis de RANKL, citoquina clave en la destrucción del hueso alveolar durante la periodontitis. Para ello, se cuanti caron los niveles de expresión de RANKL mediante PCR cuantitativa y los niveles de secreción mediante ELISA en linfocitos T activados en presencia de los serotipos capsulares K1-K6 de P. gingivalis, y estos se correlacionaron a los niveles de expresión de los factores de transcripción asociados a cada uno de los fenotipos de linfocitos efectores: Th1 (T-bet), Th2 (GATA-3), Th17 (RORC2) y Treg (Foxp3).

Resultados

Mayores niveles de expresión y secreción de RANKL fueron detectados en linfocitos T activados en presencia de los serotipos K1 y K2 de P. gingivalis, en comparación a los detectados ante los otros serotipos. Además, estos mayores niveles de RANKL se correlacionaron positivamente con los niveles de expresión de RORC2.

Conclusión

Estos datos demuestran que la síntesis de RANKL por linfocitos T se restringe a ciertos serotipos capsulares de P. gingivalis (K1 y K2) y permiten sugerir que los serotipos K1 y K2 de P. gingivalis podrían asociarse a la destrucción del hueso alveolar y a la pérdida de los dientes durante la periodontitis.

Palabras clave:
RANKL
Porphyromonas gingivalis
Th17
periodontitis
linfocitos T
Abstract
Aim

Periodontitis represents a heterogenic group of periodontal infections elicited by bacteria residing at the subgingival bio lm. Although this bio lm is constituted by a broad variety of bacterial species, only a limited number has been associated with the periodontitis aetiology, among them Porphyromonas gingivalis. P. gingivalis express a number of virulence factors that contribute to direct tissue damage; however, their pathogenicity relies mainly on the induction of a host immuno-inflammatory response. This leads to the release of a broad array of cytokines, chemokines and inflammatory mediators, which cause destruction of the tooth-supporting alveolar bone and ultimately tooth loss.

Method

In the present investigation, in order to determine whether different P. gingivalis serotypes might lead to a differential RANKL synthesis, a key cytokine involved in alveolar bone resorption, the mRNA expression and secretion of RANKL and the expression of transcription factors T-bet, GATA-3, RORC2 and Foxp3, the master-switch genes controlling the Th1, Th2, Th17, and Treg cell differentiation, respectively, were analyzed on human T cells activated with different P. gingivalis capsular (K) serotypes.

Results

T lymphocytes responding to P. gingivalis serotypes K1 or K2, but not to the other serotypes, led to an increased expression and secretion of RANKL. In addition, these higher RANKL levels correlate with RORC2 expression upon activation with K1 or K2 serotypes.

Conclusion

These data demonstrated that RANKL expression and secretion by T lymphocytes was restricted to particular P. gingivalis serotypes (namely K1 and K2), and allowed to suggest a link between these serotypes with alveolar bone destruction and teeth loosening during the periodontitis.

Key words:
RANKL
Porphyromonas gingivalis
Th17
periodontitis
T lymphocytes
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