Nicorandil cardioplegia or procaine cardioplegia?

doi:10.1016/S1010-7940(03)00384-1

HOME

HELP

FEEDBACK

SUBSCRIPTIONS

Nicorandil cardioplegia or procaine cardioplegia?

Dafvid J. Chambers*

Cardiac Surgical Research, The Rayne Institute, Guy's and St Thomas' NHS Trust, St Thomas' Hospital, London SE1 7EH, UK

Received 23 May 2003; accepted 9 June 2003.

^* Tel.: +44-207-261-0157; fax: +44-207-928-0658
e-mail: david.chambers{at}kcl.ac.uk

Key Words: Myocardial protection • Cardioplegia • Arrest

I read with interest the article by Steensrud and colleagueson myocardial protection with nicorandil cardioplegia [1]. Thestudy investigates the protective efficacy of intermittent coldblood nicorandil cardioplegia compared with intermittent standardhyperkalemic cold blood and cold crystalloid cardioplegia inpigs undergoing cardiopulmonary bypass and hearts subjectedto 60 min global ischemia and 120 min reperfusion. Measurementof function and MVO₂ demonstrated improved protection with nicorandilcardioplegia compared to either of the hyperkalemic solutions,and it is concluded that nicorandil, as sole cardioplegic agent,provides superior preservation of LV contractility and myocardialenergetics.

I disagree with the emphasis that the authors place on the importanceof nicorandil in this study. The statement that nicorandil isthe sole cardioplegic agent is incorrect; indeed, I suspect,in the context of their ‘nicorandil’ cardioplegiaformulation, that nicorandil would only have a minor cardioplegiceffect, if any, in this study. Steensrud et al. fail to acknowledgethe effect of procaine, included in their solution (albeit onlyduring the bolus initial infusion) at a concentration of 2.5mmol/L, compared with the nicorandil concentration of 0.1 mmol/L.Procaine, a Na-channel blocker, has been used as the arrestingagent in many cardioplegic solutions; a concentration of 3.7mmol/L, shown to be optimal for recovery, is close to the procaineconcentration used in this study. We have previously demonstrated[2] that Na-channel blockade (using 0.022 mmol/L tetrodotoxin),induces rapid arrest at a membrane potential of around -70 mV(thus inducing a polarized arrest) and this leads to significantlyimproved protection when compared with hyperkalemia (depolarizedarrest) in rat hearts subjected to 5 h cold (7.5 °C) globalischemia. Polarized arrest should reduce ionic imbalance andmaintain myocardial high energy phosphates (as the myocardiumrequires less energy expenditure to attempt to correct ionicchanges); we have shown [2,3] that this does indeed occur inthe polarized arrested heart compared to the depolarized heartarrested by hyperkalemia.

We have also examined the protective effects of pinacidil (aK_ATP-channel opener) as an arresting agent. Interestingly, weshowed [4] that, in hearts from various species (rat, rabbitand guinea pig), pinacidil was unable to induce arrest evenwhen infused over prolonged periods (30 min) at concentrationsup to 1.0 mmol/L. Complete arrest in guinea pig hearts couldonly be induced by a combination of pinacidil (at 0.3 mmol/L)and procaine (at 1.0 mmol/L); this combination maintained themembrane potential during arrest at approximately -70 mV andinduced protection that was significantly better than hyperkalemicarrest [4]. Studies by Sato and coworkers [5] have shown thatnicorandil, at 0.1 mmol/L (the same concentration of nicorandilused by Steensrud et al. [1]) did not influence the sarcolemmalK_ATP-channels, although mitochondrial flavoprotein oxidation(indicative of mitochondrial K_ATP-channel activation) did occur;a 10-fold higher concentration was required before sarcolemmalK_ATP-channels were opened. It is difficult to envisage, therefore,how nicorandil (at the concentration used in the study by Steensrudet al. [1]) can be exerting any effect on the sarcolemmal K_ATP-channelssufficient to induce a ‘hyperpolarization’ thatwould lead to myocardial arrest.

I believe that these authors are incorrect in suggesting thatnicorandil acts as the sole arresting agent in their ‘nicorandil’cardioplegia and that, by employing the term nicorandil cardioplegia,they are misleading the readership of the journal.

References

Steensrud T., Nordhaug D., Elvenes O.P., Korvald C., Sorlie D.G. Superior myocardial protection with nicorandil cardioplegia. Eur J Cardiothorac Surg 2003;23:670-677.[Abstract/Free Full Text]
Snabaitis A.K., Shattock M.J., Chambers D.J. Comparison of polarized and depolarized arrest in the isolated rat heart for long-term preservation. Circulation 1997;96:3148-3156.[Abstract/Free Full Text]
Snabaitis A.K., Shattock M.J., Chambers D.J. Long-term myocardial preservation: effects of hyperkalemia, sodium channel, and Na/K/2Cl cotransport inhibition on extracellular potassium accumulation during hypothermic storage. J Thorac Cardiovasc Surg 1999;118:123-134.[Abstract/Free Full Text]
Chambers D.J. Mechanisms and alternative methods of achieving cardiac arrest. Ann Thorac Surg 2003;75:S661-S666.[Abstract/Free Full Text]
Sato T., Sasaki N., O'Rourke B., Marban E. Nicorandil, a potent cardioprotective agent, acts by opening mitochondrial ATP-dependent potassium channels. J Am Coll Cardiol 2000;35:514-518.[Abstract/Free Full Text]

This Article

	Full Text (PDF)
	Erratum (v24,p1050)
	Alert me when this article is cited
	Alert me if a correction is posted
	Citation Map

Services

	Email this article to a friend
	Similar articles in this journal
	Similar articles in PubMed
	Alert me to new issues of the journal
	Add to Personal Folders
	Download to citation manager
	Permission Requests

Citing Articles

	Citing Articles via Google Scholar

Google Scholar

	Articles by Chambers, D. J.
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Chambers, D. J.

Related Collections

	Myocardial protection

Letter to the Editor

Nicorandil cardioplegia or procaine cardioplegia?