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International Journal of Pharmacology

Year: 2012 | Volume: 8 | Issue: 7 | Page No.: 647-651
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ABSTRACT

Methylsulfonylmethane (MSM) is naturally accruing organic sulphur that is known as a potent anti-inflammatory compound. The aim of this study was to investigate the effect of MSM on mRNA expressions of angiotensinogen, endothelin-1 (ET-1) and Transforming Growth Factor (TGF)-β1 in rats with monocrotaline (MCT)-induced pulmonary arterial hypertension. Wistar rats were randomly assigned to 38-days pretreatment or 28-days treatment. MSM was administered to either 10 days before or 14 days after a single dose of MCT. Right Ventricle (RV) tissue samples were obtained to evaluate changes in the inflammatory genes expression using RT-PCR assay. The expression levels of angiotensinogen, ET-1 and TGF-β1 significantly were reduced (p<0.01) at efficient dose of MSM in MCT-induced pulmonary arterial hypertensive rats. Results suggest that harmful effects of MCT induced PAH on the RV function could be attenuated by anti-inflammatory actions through the suppression of local RAAS along with associated growth-promoting factors TGF-β1 and ET-1.
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Received: June 16, 2012;   Accepted: August 23, 2012;   Published: December 31, 2012

How to cite this article

Sadollah Mohammadi, Alireza Garjani, Moslem Najafi, Hossein Hamzeiy, Nasrin Maleki-Dizaji, Yadollah Omidi, Shabnam Fayezi, Masoud Darabi, Sara Mostafalou, Kambiz Hassanzadeh and Sajjad Khani, 2012. Inhibitory Effects of Methylsulfonylmethane on Ventricular Hypertrophy Related Gene Expression. International Journal of Pharmacology, 8: 647-651.

DOI: 10.3923/ijp.2012.647.651

URL: https://scialert.net/abstract/?doi=ijp.2012.647.651

INTRODUCTION

Pulmonary Arterial Hypertension (PAH) is a pathophysiological state characterized by a progressive increase in pulmonary vascular resistance. In addition to inducing myocardial hypertrophy, it also induces marked interstitial fibrosis to compensate for the increased ventricular workload. These adaptive changes often clinically lead to heart failure and sudden cardiac death (Simonneau et al., 2009). Despite all, current progress in the diagnosis and therapeutics, PAH continues to be a devastating disease with a high morbidity and mortality (Benza et al., 2010). Angiotensin II has been recognized as an important contributor to cardiac hypertrophy and inflammation in PAH (Huggins et al., 2003). Angiotensin II increases endothelin 1 (ET-1) expression which stimulates the conversion of angiotensinogen to angiotensin II and promotes myocardial inflammation by recruiting leukocytes and releasing of fibrogenic cytokines, like Transforming Growth Factor (TGF)-β (Gray et al., 1998; Jun et al., 2007). Angiotensin II also up-regulates TGF-β synthesis by cardiac fibroblasts occurring due to systemic hypertension (Huntgeburth et al., 2011).

Methylsulfonylmethane (MSM) is naturally occurring organic sulphur that is known as a potent anti-oxidant/anti-inflammatory compound (Beilke et al., 1987; Ebisuzaki, 2003). MSM is widely used as an arthritis remedy with inhibitory activities on proinflammatory cytokines (Alam and Layman, 1983; Debbi et al., 2011). Despite, an increasing clinical use, the mechanisms by which MSM exert their effects remain largely unknown.

Recent findings have linked anti-inflammatory effects of MSM to modifications in proinflammatory gene expression. Kim et al. (2009) have recently shown that MSM inhibits LPS-induced release of pro-inflammatory mediators in macrophages through downregulation of NF-κB signaling. MSM may also be beneficial in PAH due to its anti-inflammatory and anti-proliferative effects (Lim et al., 2012). It has been shown that sulfur dioxide (SO2) and its derivatives play a protective role in PAH (Jin et al., 2008). Thus, it is possible that MSM exerts its effect on PAH by interfering with inflammatory processes that may be associated with the heart failure. Monocrotaline (MCT) is a toxic pyrrolizidine alkaloid and has a selective toxic effect on pulmonary vessels without an effect on systemic vessels. To investigate whether MSM may provide therapeutic or preventive effects on PAH, an experimental study was conducted examining the gene expression of the angiotensinogen, ET-1 and TGF-β1 in the Right Ventricles (RV) from rats with MCT-induced PAH subjected to pretreatment or post treatment.

MATERIALS AND METHODS

Animals: Two-month-old male Wistar rats (200±20 g) were, fed with standard laboratory chow ad libitum, used in the experiment, as previously described by (Garjani et al., 2009). Animals obtained from the Pasteur Institute of Iran (Tehran, Iran). Tabriz University of Medical Sciences animal ethics committee approved the study protocol. Injections were all administered intraperitoneally (i.p.) to rats. Invasive experimental procedures were carried out on pentobarbital anaesthetized rats (60 mg kg-1 b.wt. i.p.). RV tissue samples were harvested and snap frozen in liquid nitrogen for further RT-PCR analysis of angiotensinogen, ET-1 and TGF-β1 genes.

Experimental protocols: MCT (Sigma, MO, USA) was dissolved in 1 M HCl, diluted with physiologic saline and neutralized to pH 7.4 with 1 M NaOH. MSM (Sigma, MO, USA) used for systemic administration were dissolved in physiological saline. PAH was induced by means of a single dose of MCT (60 mg kg-1). The effective dose of MSM was determined according to a significant improvement in hemodynamic status of MCT-induced PAH rats. In a separate series of experiments, rats were subjected to post-treatment with MSM (400 mg kg-1 day-1) from the third week after injection of MCT (MSM-post treated group, n = 22) or pre-treatment with MSM (400 mg kg-1 day-1) from the 10th day prior to injection of MCT and for 4 weeks after the MCT (MSM-pretreated group, n = 22). Saline was used as vehicle in control experiments. MSM was well tolerated by the rats and no abnormal behavior was observed.

RT-PCR analysis: Total RNAs were purified with trizol reagent (Invitrogen, Carlsbad, CA). One microgram of RNA was reverse-transcribed using the First Strand (Promega, Madison, WI) as per the manufacturer’s instructions. Semiquantitation of the cDNA was performed by RT-PCR using specific primers (Table 1) according to a previous report (Park et al., 2001). The reverse transcripts of candidate genes were amplified with GAPDH as an internal control, using standard conditions of PCR.

Quantitative analysis: For comparing the amount of PCR product between samples, a gel digitizing software, Uviphotomw (UVItec, Cambridge, UK; version 11.01), was used for estimating the intensity of each band on the gel. Each experiment was repeated four times. The Coefficients of Variation (CV) were about 5-8%.

Statistical analysis: Data presented are the Mean±SD of four separate experiments. Calculation of significance between groups was done according to Student’s t-test and a p-value <0.05 was considered statistically significant.

RESULTS

To explore possible mechanisms by which development of PAH is inhibited by MSM treatment, at a dose effective in significantly improving hemodynamic (data not shown); the effects of MSM pretreatment and posttreatment on mRNA expressions of the angiotensinogen, ET-1 and TGF-β1 were examined in MCT-induced pulmonary hypertensive rats. Levels of angiotensinogen, ET-1 and TGF-β1 mRNAs in the hypertrophied RV were significantly increased at week 4 of MCT treatment. The angiotensinogen, ET-1 and TGF-β1 mRNAs levels were significantly decreased in both MSM-pretreated and -post treated rats when compared with those in the saline-treated pulmonary hypertensive rats (p<0.05; Fig. 1). Levels of ET-1 mRNA transcript in MSM-treated pulmonary hypertensive rats decreased, even as compared to the values corresponding to normotensive control rats (p<0.01; Fig. 1).

Table 1: Primer sequences used for reverse transcription-polymerase chain reaction (RT-PCR)
Image for - Inhibitory Effects of Methylsulfonylmethane on Ventricular Hypertrophy Related Gene Expression

Image for - Inhibitory Effects of Methylsulfonylmethane on Ventricular Hypertrophy Related Gene Expression
Fig. 1(a-c): Effects of methylsulfonylmethane on right ventricle (RV) hypertrophy related gene expression of (a) Angiotensinogen, (b) Transforming growth factor (TGF)-β1, (c) Endothelin-1 (ET-1), RV tissue samples were harvested 28 days after MCT administration and processed for RT-PCR analysis. The mean values±SD of four independent experiments are given. *p<0.01 via student’s t-test, MCT: Monocrotaline, MSM: Methylsulfonylmethane

DISCUSSION

In this study, significant changes in angiotensinogen, ET-1 and TGF-β1 gene expression were observed in MCT-induced pulmonary hypertensive rats and these changes were reduced with MSM in two distinct experimental treatments for the first time. Consistent with these findings, several studies have reported that cardiovascular system of MCT-induced pulmonary hypertensive rats showed inflammatory alterations similar to those observed in human PAH (Akhavein et al., 2007). The effects of PAH on myocardium include hypertrophy and interstitial inflammatory cell infiltration. The RV tissue in the rat model of PAH was generally characterized by inflammatory reaction and showed alterations in contractile and regulatory protein expression (Bogaard et al., 2009). The expression changes observed in patients with chronic heart failure included markedly increased serum levels and myocyte expression of the pro-inflammatory cytokines Tumor Necrosis Factor (TNF)-α, interleukin (IL)-1 and IL-6 (Bogaard et al., 2009).

In this study, gene expression investigations showed elevated angiotensinogen, ET-1 and TGF-β1 in RV myocardium of PAH rats compared with control. A similar observation was previously made by Park et al. (2001) in another study of gene expression patterns in rats with RV hypertrophy. The Renin-angiotensin-aldosterone System (RAAS) is deregulated in PAH and suggested to potentially contribute to the pathogenesis of PAH. Both ET-1 and TGF-β1 are autocrine/paracrine growth factors and mediate ventricular dysfunction associated with elevated RAAS activity (Rosenkranz, 2004).

The mechanism for toxic effects of MCT on the lung has not yet been fully explained. MCT itself can affect adversely metabolic activity in vitro (Fu et al., 2004). However, as the animal model of PAH is induced using a single-dose over several weeks it seems unlikely that MCT contributes to such an effect in vivo. In animals exposed to agents that induce inflammation, MSM provides substantial protection against tissue destruction and chronic inflammation (Amirshahrokhi et al., 2011). In addition, MSM has been shown to protect against undesirable inflammatory state induced by exposure to PS, potent allergens and certain parasitic infections (Barrager et al., 2002; Kim et al., 2009). Comparable results were observed in the present study as angiotensinogen, ET-1 and TGF-β1 gene expression were increased in MCT-induced pulmonary hypertensive rats and these alterations decreased following treatment with MSM.

In this study, ET-1 expression level was lower in the RV tissue homogenates of MSM-treated pulmonary hypertensive rats than in either the normotensive controls or the MCT-induced pulmonary hypertensive rats. Similarly, An elevated level of ET-1 in plasma and lung tissues of pulmonary arterial hypertension patients has been detected (Giaid et al., 1993) and the endothelin receptor antagonists have been suggested as effective treatments for this condition (Channick et al., 2001; Garjani et al., 1995). According to study results, MSM was found to prevent and reverse effectively ET-1 response in MCT-induced PAH. These results are consistent with previous reports showing antiinflammatory effects of MSM through inhibition of proinflammatory cytokine production (Kim et al., 2009).

Previous clinical and experimental reports have implicated increased oxidative stress as a mediator in the pathogenesis and the development of PAH (Farahmand et al., 2004; Li et al., 2002). Accordingly, antioxidant therapy has been effective in the treatment of RV dysfunction in PAH (Redout et al., 2010). RAAS and ET-1 are known as prooxidant agents that induce Reactive Oxygen Species (ROS) production through the activation of ROS-generating enzymes (Cheng et al., 2003; Touyz et al., 2004). The finding of increased RAAS and ET-1 in rats with MCT-induced pulmonary hypertension supports the presence of enhanced oxidative stress in the RV of PAH rats. The PAH-induced increase in RAAS and ET-1 were reverted by pre- and post-treatment of MSM, indicating an improvement in the oxidative status of the cells. Moreover, MSM has been shown to act directly as free radical scavenger which would further add to the efficiency of MSM as an antioxidant (Parcell, 2002).

In both pre- and post-treatment assessments, a decrease in transcriptional elevation of proinflammatory agents with MSM treatment was evident. No documented evidence is available regarding the effect of MSM on inflammation-related parameters in myocardial tissue of pulmonary hypertensive rats. Although, no mechanistic interpretation can be made at this point, the results obtained in the present study provide evidence for the first time that the MSM could limit inflammatory response in the RV following to pulmonary hypertension. However, the experimental model used in this study may not be analogous to the clinical situation and could not be used in a clinical setting. Future studies to clarify how MSM affects RV function will help in designing MSM therapy for the treatment of PAH.

CONCLUSION

In conclusion, these results suggest that MCT-induced PAH could induce harmful effects on the RV function, probably due to an increase in proinflammatory molecules and oxidative damage. In addition, it was demonstrated that MSM could exert protective antiinflammatory effects through the suppression of local RAAS along with associated growth-promoting factors, such as TGF-β1 and ET-1.

ACKNOWLEDGMENT

This study was partially supported by a grant from the Tabriz University of Medical Sciences (1388/4/20-5/4/3255) to AG.

REFERENCES

  1. Simonneau, G., I.M. Robbins, M. Beghetti, R.N. Channick and M. Delcroix et al., 2009. Updated clinical classification of pulmonary hypertension. J. Am. Coll. Cardiol., 54: S43-S54.
    PubMed
  2. Benza, R.L., D.P. Miller, M. Gomberg-Maitland, R.P. Frantz and A.J. Foreman et al., 2010. Predicting survival in pulmonary arterial hypertension: insights from the registry to evaluate early and long-term pulmonary arterial hypertension disease management (REVEAL). Circulation, 122: 164-172.
    CrossRefDirect Link
  3. Huggins, C.E., A.A. Domenighetti, T. Pedrazzini, S. Pepe and L.M. Delbridge, 2003. Elevated intracardiac angiotensin ii leads to cardiac hypertrophy and mechanical dysfunction in normotensive mice. J. Renin. Angiotensin. Aldosterone. Syst., 4: 186-190.
    CrossRef
  4. Gray, M.O., C.S. Long, J.E. Kalinyak, H.T. Li and J.S. Karliner, 1998. Angiotensin II stimulates cardiac myocyte hypertrophy via paracrine release of TGF-Beta1 and endothelin-1 from fibroblasts. Cardiovasc. Res., 40: 352-363.
    Direct Link
  5. Jun, T., Z. Liancai and W. Bochu, 2007. Effect of ginsenosides on malondialdehyde, nitric oxide and endothelin-1 production in vascular endothelial cells suffering from lipid peroxidation injury. Int. J. Pharmacol., 3: 101-105.
    CrossRefDirect Link
  6. Huntgeburth, M., K. Tiemann, R. Shahverdyan, K.D. Schluter and R. Schreckenberg et al., 2011. Transforming growth factor beta oppositely regulates the hypertrophic and contractile response to beta-adrenergic stimulation in the heart. PLoS One., Vol 6.
    Direct Link
  7. Ebisuzaki, K., 2003. Aspirin and methylsulfonylmethane (MSM): A search for common mechanisms, with implications for cancer prevention. Anticancer Res., 23: 453-458.
    PubMed
  8. Beilke, M.A., C. Collins-Lech and P.G. Sohnle, 1987. Effects of dimethyl sulfoxide on the oxidative function of human neutrophils. J. Lab Clin. Med., 110: 91-96.
    PubMed
  9. Alam, S.S. and D.L. Layman, 1983. Dimethyl sulfoxide inhibition of prostacyclin production in cultured aortic endothelial cells. Ann. N. Y. Acad. Sci., 411: 318-320.
    PubMed
  10. Debbi, E.M., G. Agar, G. Fichman, Y.B. Ziv and R. Kardosh et al., 2011. Efficacy of methylsulfonylmethane supplementation on osteoarthritis of the knee: A randomized controlled study. BMC Complement Altern. Med., 11: 50-53.
    CrossRef
  11. Kim, Y.H., D.H. Kim, H. Lim, D.Y. Baek, H.K. Shin and J.K. Kim, 2009. The anti-inflammatory effects of methylsulfonylmethane on lipopolysaccharide-induced inflammatory responses in murine macrophages. Biol. Pharm. Bull., 32: 651-656.
    PubMed
  12. Lim, E.J., D.Y. Hong, J.H. Park, Y.H. Joung and P. Darvin et al., 2012. Methylsulfonylmethane suppresses breast cancer growth by down-regulating STAT3 and STAT5b pathways. PLoS One, Vol. 7.
    Direct Link
  13. Jin, H.F., S.X. Du, X. Zhao, H.L. Wei and Y.F. Wang et al., 2008. Effects of endogenous sulfur dioxide on monocrotaline-induced pulmonary hypertension in rats. Acta Pharmacol. Sin., 29: 1157-1166.
    CrossRef
  14. Akhavein, F., E.J. St-Michel, E. Seifert and C.V. Rohlicek, 2007. Decreased left ventricular function, myocarditis, and coronary arteriolar medial thickening following monocrotaline administration in adult rats. J. Applied Physiol., 103: 287-295.
    PubMed
  15. Bogaard, H.J., K. Abe, A. Vonk Noordegraaf and N.F. Voelkel, 2009. The right ventricle under pressure: cellular and molecular mechanisms of right-heart failure in pulmonary hypertension. Chest, 135: 794-804.
    PubMed
  16. Park, H.K., S.J. Park, C.S. Kim, Y.W. Paek, J.U. Lee and W.J. Lee, 2001. Enhanced gene expression of renin-angiotensin system, tgf-beta1, endothelin-1 and nitric oxide synthase in right-ventricular hypertrophy. Pharmacol. Res., 43: 265-273.
    PubMed
  17. Rosenkranz, S., 2004. TGF-β1 and angiotensin networking in cardiac remodeling. Cardiovasc. Res., 63: 423-432.
    PubMed
  18. Fu, P.P., Q. Xia, G. Lin and M.W. Chou, 2004. Pyrrolizidine alkaloids-genotoxicity, metabolism enzymes, metabolic activation and mechanisms. Drug Metab. Rev., 36: 1-55.
    PubMed
  19. Amirshahrokhi, K., S. Bohlooli and M.M. Chinifroush, 2011. The effect of methylsulfonylmethane on the experimental colitis in the rat. Toxicol. Applied Pharmacol., 253: 197-202.
    PubMed
  20. Barrager, E., J.R. Jr. Veltmann, A.G. Schauss and R.N. Schiller, 2002. A multicentered, open-label trial on the safety and efficacy of methylsulfonylmethane in the treatment of seasonal allergic rhinitis. J. Altern. Complement Med., 8: 167-173.
    CrossRefPubMed
  21. Giaid, A., M. Yanagisawa, D. Langleben, R.P. Michel and R. Levy et al., 1993. Expression of endothelin-1 in the lungs of patients with pulmonary hypertension. N. Engl. J. Med., 328: 1732-1739.
    Direct Link
  22. Channick, R.N., G. Simonneau, O. Sitbon, I.M. Robbins and A. Frost et al., 2001. Effects of the dual endothelin-receptor antagonist bosentan in patients with pulmonary hypertension: A randomised placebo-controlled study. Lancet, 358: 1119-1123.
    CrossRefPubMed
  23. Garjani, A., C.L. Wainwright, I.J. Zeitlin, C. Wilson and S.J. Slee, 1995. Effects of endothelin-1 and the ETA-receptor antagonist, BQ123, on ischemic arrhythmias in anesthetized rats. J. Cardiovasc Pharmacol., 25: 634-642.
    PubMed
  24. Farahmand, F., M.F. Hill and P.K. Singal, 2004. Antioxidant and oxidative stress changes in experimental cor pulmonale. Mol. Cell Biochem., 260: 21-29.
    PubMed
  25. Li, J.M., N.P. Gall, D.J. Grieve, M. Chen and A.M. Shah, 2002. Activation of NADPH oxidase during progression of cardiac hypertrophy to failure. Hypertension, 40: 477-484.
    PubMed
  26. Redout, E.M., A. van der Toorn, M.J. Zuidwijk, C.W. van de Kolk and C.J. van Echteld et al., 2010. Antioxidant treatment attenuates pulmonary arterial hypertension-induced heart failure. Am. J. Physiol. Heart Circ. Physiol., 298: H1038-H1047.
    CrossRefDirect Link
  27. Cheng, T.H., P.Y. Cheng, N.L. Shih, I.B. Chen, D.L. Wang and J.J. Chen, 2003. Involvement of reactive oxygen species in angiotensin ii-induced endothelin-1 gene expression in rat cardiac fibroblasts. J. Am. Coll. Cardiol., 42 : 1845-1854.
    CrossRefDirect Link
  28. Touyz, R.M., G. Yao, E. Viel, F. Amiri and E.L. Schiffrin, 2004. Angiotensin II and endothelin-1 regulate map kinases through different redox-dependent mechanisms in human vascular smooth muscle cells. J. Hypertens, 22: 1141-1149.
    PubMed
  29. Parcell, S., 2002. Sulfur in human nutrition and applications in medicine. Altern. Med. Rev., 7: 22-44.
    PubMedDirect Link
  30. Garjani, A., A. Afrooziyan, H. Nazemiyeh, M. Najafi, A. Kharazmkia and N. Maleki-Dizaji, 2009. Protective effects of hydroalcoholic extract from rhizomes of Cynodon dactylon (L.) Pers. on compensated right heart failure in rats. BMC Complement Altern. Med., 9: 28-32.
    CrossRef

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