MTA preparations from different origins may vary in their antimicrobial activity

Khalid Al-Hezaimi; Thakib A Al-Shalan; Jafar Naghshbandi; James H S Simon; Ilan Rotstein

doi:10.1016/j.tripleo.2009.01.045

MTA preparations from different origins may vary in their antimicrobial activity

Oral Surg Oral Med Oral Pathol Oral Radiol Endod. 2009 May;107(5):e85-8. doi: 10.1016/j.tripleo.2009.01.045.

Authors

Khalid Al-Hezaimi¹, Thakib A Al-Shalan, Jafar Naghshbandi, James H S Simon, Ilan Rotstein

Affiliation

¹ King Saud University, College of Dentistry, Riyadh, Saudi Arabia. alhezaim@usc.edu

PMID: 19426914
DOI: 10.1016/j.tripleo.2009.01.045

Abstract

Objective: The antimicrobial effects of 4 mineral trioxide aggregate (MTA) preparations, 2 white-colored (WMTA-1, WMTA-2) and 2 gray-colored (GMTA-1, GMTA-2), against C. albicans and E. faecalis were assessed in vitro.

Methodology: Minimal inhibitory concentration (MIC) for each preparation was determined using the tube dilution test and Sabouraud agar media for C. albicans and brain heart infusion media for E. faecalis. Broth tubes were prepared and divided into experimental and control groups. Aliquots of each of the tested microorganisms were taken from a stock culture and added to each experimental and positive control group. All groups were incubated at 37 degrees C and evaluated for turbidity at 24-, 48-, and 72-hour time periods. Samples of 0.1 mL from each of the experimental and control tubes were subcultured on agar or brain heart infusion plates to confirm visible signs of bacterial or fungal growth.

Results: MIC of MTA against the 2 microorganisms tested varied among the 4 preparations tested. WMTA-1 and WMTA-2 inhibited C. albicans growth at concentrations of 3.125 mg/10 mL and 25 mg/10 mL, respectively, and statistically significant differences were found between WMTA-1 and WMTA-2 (P < .001). WMTA-1 and WMTA-2 inhibited E. faecalis growth at concentrations of 12.5 mg/10 mL and 50 mg/10 mL, respectively, and statistically significant differences were found between WMTA-1 and WMTA-2 (P < .001). GMTA-1 and GMTA-2 inhibited E. faecalis growth at concentrations of 12.5 mg/10 mL and 3.125 mg/10 mL, respectively, and statistically significant differences were found between GMTA-1 and GMTA-2 (P < .001). Both GMTA-1 and GMTA-2 inhibited C. albicans growth at a concentration of 3.125 mg/10 mL and no statistical differences were found between the preparations. Subculture of the broth tubes in agar or brain heart infusion plates confirmed the turbidity test result.

Conclusion: The origin of MTA as well as the type of preparation may affect its antimicrobial characteristics. Clinicians should be aware of variations that may exist among such MTA preparations.

Publication types

Comparative Study
Research Support, Non-U.S. Gov't

MeSH terms

Aluminum Compounds / chemistry
Aluminum Compounds / pharmacology*
Calcium Compounds / chemistry
Calcium Compounds / pharmacology*
Candida albicans / drug effects*
Colony Count, Microbial
Drug Combinations
Enterococcus faecalis / drug effects*
France
Germany
Microbial Sensitivity Tests
Oxides / chemistry
Oxides / pharmacology*
Root Canal Filling Materials / chemistry
Root Canal Filling Materials / pharmacology*
Silicates / chemistry
Silicates / pharmacology*

Substances

Aluminum Compounds
Calcium Compounds
Drug Combinations
Oxides
Root Canal Filling Materials
Silicates
mineral trioxide aggregate