Exploring the Role of Long Non-Coding Rnas in Periodontitis

Exploring the Role of Long Non-Coding Rnas in Periodontitis Publisher

Sayad A¹ ; Taheri M² ; Sadeghpour S³ ; Omrani MD³ ; Shams B⁴ ; Mirzajani S⁵ ; Arsangjang S⁶ ; Houshmand B⁴ ; Amid R⁴ ; Gholami L^{1, 7} ; Ghafourifard S³

Show Affiliations

1. Dental Research Center, Research Institute for Dental Sciences, Dental School, Shahid Beheshti University of Medical Sciences, Tehran, Iran
2. Urogenital Stem Cell Research Center, Shahid Beheshti University of Medical Sciences, Tehran, Iran
3. Department of Medical Genetics, Shahid Beheshti University of Medical Sciences, Tehran, Iran
4. Department of Periodontics, School of Dentistry, Shahid Beheshti University of Medical Sciences, Tehran, Iran
5. Pediatric Cell Therapy Research Center, Tehran University of Medical Sciences, Tehran, Iran
6. Department of Biostatistics and Epidemiology, Cancer Gene Therapy Research Center, Faculty of Medicine, Zanjan University of Medical Sciences, Zanjan, Iran
7. Department of Periodontics, School of Dentistry, Hamadan University of Medical Sciences, Hamadan, Iran

Source: Meta Gene Published:2020

Abstract

Recent studies have underscored the role of long non-coding RNAs (lncRNAs) in the pathophysiology of several immune-related conditions such as periodontitis. In the current study, we aimed at exploration of the role of four lncRNAs (UCA1, NEAT1, FAS-AS1 and NKILA) in this disorder. We compared expression of these genes between blood and gingival samples obtained from patients with periodontitis and normal subjects. Expression of UCA1 was significantly lower in peripheral blood of patients compared with controls (Posterior beta of RE = −2.069, P value = .029). When dividing samples based on the gender of individuals, the difference was significant between female patients and female controls (Posterior beta of RE = -1.895, P value = .049), but not between male subjects. There was no significant difference in tissue expression of UCA1 between cases and controls. Expression of FAS-AS1 was significantly lower in peripheral blood of patients compared with controls (Posterior beta of RE = -7.065, P value = .001). The difference was significant among both male and female patients versus sex-matched controls (Posterior beta of RE = -8.166, P value = .006 and Posterior beta of RE = -5.118, P value = .026, respectively). Yet, expression of this lncRNA was not different between tissues samples obtained from patients and controls. Expression of NEAT1 was significantly higher in tissue samples obtained from patients compared with controls (Posterior beta of RE = 3.386, P value = .043). Such pattern was also observed in tissue samples obtained from male persons (Posterior beta of RE = 6.417, P value = .017) but not female persons. Surprisingly, expression of NEAT1 was lower in patients' blood samples compared with controls (Posterior beta of RE = -2.99, P value = .01) and in blood samples obtained from female patients compared with sex-matched controls (Posterior beta of RE = -2.991, P value = .01). Expression of NKILA was significantly higher in both tissue samples and blood samples obtained from patients compared with controls (Posterior beta of RE = 7.974, P value<.0001 and Posterior beta of RE = 5.122, P value = .001). Difference in tissue expression of this lncRNA was significant in both male and female patients compared with sex-matched controls, but blood expression of this lncRNA was only different between female patients and female controls. There were significant correlations between tissue expressions of UCA1 and NEAT1 (r = 0.79, P < .001), tissue expressions of FAS-AS1 and NEAT1 (r = 0.76, P < .001) and blood expressions of UCA1 and NEAT1 (r = 0.75, P < .001) in patients with periodontitis. The current study supports the role of lncRNAs in the pathophysiology of periodontitis and potentiates them as putative biomarkers for this disorder. © 2020 Elsevier B.V.

2. The Emerging Role of Lncrnas in Multiple Sclerosis, Journal of Neuroimmunology (2020)

3. Emerging Role of Long Non-Coding Rnas in the Pathogenesis of Periodontitis, Biomedicine and Pharmacotherapy (2020)

4. Expression Analysis of Nf-Κb-Associated Long Noncoding Rnas in Peripheral Blood Mononuclear Cells From Relapsing-Remitting Multiple Sclerosis Patients, Journal of Neuroimmunology (2021)

Experts (# of related papers)

Abdolreaza Naser Moghadasi (1)

Style	Citing Format
MLA	Sayad A, et al.. "Exploring the Role of Long Non-Coding Rnas in Periodontitis." Meta Gene, vol. 24, no. , 2020, pp. -.
APA	Sayad A, Taheri M, Sadeghpour S, Omrani MD, Shams B, Mirzajani S, Arsangjang S, Houshmand B, Amid R, Gholami L, Ghafourifard S (2020). Exploring the Role of Long Non-Coding Rnas in Periodontitis. Meta Gene, 24(), -.
Chicago	Sayad A, Taheri M, Sadeghpour S, Omrani MD, Shams B, Mirzajani S, Arsangjang S, et al.. "Exploring the Role of Long Non-Coding Rnas in Periodontitis." Meta Gene 24, no. (2020): -.
Harvard	Sayad A et al. (2020) 'Exploring the Role of Long Non-Coding Rnas in Periodontitis', Meta Gene, 24(), pp. -.
Vancouver	Sayad A, Taheri M, Sadeghpour S, Omrani MD, Shams B, Mirzajani S, et al.. Exploring the Role of Long Non-Coding Rnas in Periodontitis. Meta Gene. 2020;24():-.
BibTex	@article{ author = {Sayad A and Taheri M and Sadeghpour S and Omrani MD and Shams B and Mirzajani S and Arsangjang S and Houshmand B and Amid R and Gholami L and Ghafourifard S}, title = {Exploring the Role of Long Non-Coding Rnas in Periodontitis}, journal = {Meta Gene}, volume = {24}, number = {}, pages = {-}, year = {2020} }
RIS	TY - JOUR AU - Sayad A AU - Taheri M AU - Sadeghpour S AU - Omrani MD AU - Shams B AU - Mirzajani S AU - Arsangjang S AU - Houshmand B AU - Amid R AU - Gholami L AU - Ghafourifard S TI - Exploring the Role of Long Non-Coding Rnas in Periodontitis JO - Meta Gene VL - 24 IS - SP - EP - PY - 2020 ER -

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