We read with great interest the recent results from ESC-EORP
Registry of Pregnancy and Cardiac disease (ROPAC), concerning pregnancy.
outcomes in women with systemic right ventricle (sRV) and transposition of the
great arteries (TGA) by Tutarel et al. (1) In Tutarel et al. analysis HF was the
most frequent maternal complication (9.1%). These results are concordant
with our previous observations of 24 pregnancies of women with TGA after
atrial switch operation and matched non-pregnant controls with TGA after atrial
redirection. 2 In our series 2 women deteriorated from the functional NYHA
class I to II after the first pregnancy and one woman in her fourth pregnancy
deteriorated from class I to III. Tutarel’s results reinforce our conclusion that,
from a cardiologist’s point of view, pregnancy after the Mustard/Senning
operation was relatively well-tolerated and safe.
In ROPAC study the information on tricuspid regurgitation (TR) was collected, but was
not mandatory. Therefore Tutarel et al. concluded that dedicated studies focusing on
sRV function and TR are warranted. Our dataset provided relevant information
on sRV and TR. At baseline, all women had preserved or only mildly reduced
sRV function estimated by echocardiography before pregnancy and absent or
mild TR. There were no differences between non-pregnant matched controls
and pregnant women in sRV function, degree of TR, at the last follow-up visit
(mean follow-up period 80 ± 57 months for pregnant group versus 84 ± 49
months for nulliparous controls (P=NS). Significant deterioration of tricuspid
regurgitation (from mild to moderate) was observed in one pregnant woman
(after fourth pregnancy) and in one nulliparous woman. Increase in TR severity
was not accompanied by a significant reduction of sRV systolic function evaluated by
echocardiography.
References
1. Tutarel O, Baris L, Budts W, et al
Pregnancy outcomes in women with a systemic right ventricle and transposition of the great arteries results from the ESC-EORP Registry of Pregnancy and Cardiac disease (ROPAC)
Heart Published Online First: 28 April 2021. doi: 10.1136/heartjnl-2020-318685
2. Lipczynska M, Szymanski P, Trojnarska O, et al. Pregnancy in women with complete transposition of the great arteries following the atrial switch procedure. A study from three of the largest Adult Congenital Heart Disease centers in Poland, The Journal of Maternal-Fetal & Neonatal Medicine, DOI:10.1080/14767058.2016.1177821

Sodium-glucose co-transporter 2 inhibitors with cellular anti-ischemics: A favorable combination in diabetic patients with cardiovascular disease

Kenan YALTA, MD a
Ugur OZKAN, MD a
Tulin YALTA, MD b

a,TrakyaUniversity, CardiologyDepartment, Edirne, TURKEY
b,TrakyaUniversity, Pathology Department, Edirne, TURKEY
Corresponding Author: Kenan YALTA Trakya University, CardiologyDepartment, Edirne, TURKEY
Email- kyalta@gmail.com, akenanyalta@trakya.edu.tr Phone: 00905056579856

Sodium-glucose co-transporter 2 (SGLT2) inhibitor therapy is a specific mode of anti-diabetic strategy that significantly improves cardiovascular outcomes (1). The recently published article by Joshi SS, et al (1) has focused on beneficial effects of SGLT2 inhibitors in the setting of heart failure (HF). We fully agree that complex cellular mechanisms, beyond diuresis (1), seem to underlie pleitrophic actions of these agents. More specifically, it also seems likely that SGLT2 inhibitors might potentiate favorable effects of certain metabolic agents including cellular anti-ischemics (and vice versa) in diabetic patients with cardiovascular disease. Accordingly, combination of SGLT2 inhibitors with cellular anti-ischemic regimens might have important implications in these patients:
It is well known that free fatty acids (FFAs) serve as the major energy source in myocardium under physiological conditions (1). However, a significant shift to oxidation of more energy-efficient substrates (including glucose and ketone bodies) usually takes place in the setting of myocardial ischemia and/or failure (2). Moreover, this shift is expected to be even more pronounced under certain medications including cellular anti-ischemics (trimetazidine, etc.) that exert their actions largely through inhibition of FFA oxidation (3). In a recent meta-analysis comprising diabetic patients, trimetazidine was demonstrated to exert favorable effects including improvement in left ventricular systolic functions, myocardial ischemic episodes and serum glucose parameters (fasting glucose and HbA1C), etc. largely attributable to its metabolic, anti-oxidant and anti-hyperglycemic effects in these patients (3). However, impaired myocardial uptake of glucose in diabetic patients (1-3) potentially hinders maximum therapeutic benefits of cellular anti-ischemics during periods of heightened metabolic demand. This signifies the need for alternative energy-efficient substrates (including ketone bodies) in diabetic patients receiving cellular anti-ischemics.
In this context, SGLT2 inhibitors provide sufficient amounts of circulating ketone bodies (1) that seem to maximize actions of cellular anti-ischemics on myocardial energetics in diabetic patients. Moreover, hyperketonemia associated with SGLT2 inhibitors (1) might also prevent excessive uptake of FFAs (a reactive phenomenon predisposing to diabetic cardiomyopathy due to lipotoxicity (2)) potentially associated with the use of cellular anti-ischemics in diabetic patients. On the other hand, cellular anti-ischemics might possibly heighten favorable impact of SGLT2 inhibitors mostly through their metabolic actions (increased insulin sensitivity due to translocation of GLUT4 ,etc. (3)) and anti-oxidant features (that might reverse myocardial remodeling (3)). Accordingly, combined use of certain metabolic agents including SGLT2 inhibitors, dichloroacetate, perhexiline, trimetazidine, etc. , was previously suggested as a potential strategy to combat failing myocardium (yet; with no recommendation of a particular combination) (4). In this regard, combination of SGLT2 inhibitors and trimetazidine seems to be a promising option (due to the mutually complementary actions of these agents).
In summary, concomitant use of cellular anti-ischemics and SGLT2 inhibitors might result in a synergistic therapeutic benefit in diabetic patients with cardiovascular disease (HF and coronary syndromes). However, this needs to be tested in clinical trials.
Conflict of Interest: None

References:
1- Joshi SS, Singh T, Newby DE, Singh J. Sodium-glucose co-transporter 2 inhibitor therapy: mechanisms of action in heart failure. Heart. 2021 Feb 26:heartjnl-2020-318060. doi: 10.1136/heartjnl-2020-318060. Epub ahead of print. PMID: 33637556
2- García-Ropero Á, Vargas-Delgado AP, Santos-Gallego CG, Badimon JJ. Inhibition of Sodium Glucose Cotransporters Improves Cardiac Performance. Int J Mol Sci. 2019; 20(13): 3289. doi: 10.3390/ijms20133289. PMID: 31277431; PMCID: PMC6651487.
3- Lin Y, Wang ZL, Yan M, Zhu FY, Duan Y, Sun ZQ. Effect of Trimetazidine on Diabetic Patients with Coronary Heart Diseases: A Meta-Analysis of Randomized, Controlled Trials. Chin Med Sci J. 2020; 35(3): 226-238.
4- Hamilton DJ. Metabolic Recovery of the Failing Heart: Emerging Therapeutic Options. Methodist Debakey Cardiovasc J. 2017; 13(1): 25-28. doi: 10.14797/mdcj-13-1-25. PMID: 28413579; PMCID: PMC5385791.

The management of hypertension generates huge opportunities for opportunistic screening for atrial fibrillation(AF). To maximise that opportunity documentation of regularity of the pulse and, hence, for AF, should be routine at each visit to primary care or to secondary care. Furthermore, that should be the routine during follow up visits of patients with known hypertension. The rationale is that hypertension is a recognised risk factor for incident AF(1), and for progression of paroxysmal AF to permanent AF(2). thereby mandating a recognition that patients with known hypertension should be allocated to a high risk subgroup in whom opportunistic screening for AF should be maximised. There are opportunities for AF screening even with home blood pressure measurement. Some self blood pressure measuring devices trigger an alert when there is an irregularity in the pulse. Patients should be educated to inform their doctor when such alerts occur so that the patient can be evaluated further by electrocardiography.
The treatment phase of hypertension addresses the challenge of atrial fibrillation by mitigating the risk of new onset development of that arrhythmia. Using data from SPRINT(Systolic Blood Pressure Intervention Trial) Soliman et al showed that intensive blood pressure lowering to a systolic blood pressure of < 120 mm Hg was associated with a 26% lower risk of developing new AF(hazard ratio, 0.74[95% Confidence Interval, 0.56-0.98]; P=0.37(3). What now needs to be recognised as the next challenge is to identify which one of the antihypertensive drug classes optimally mitigates the risk of new-onset AF. In conclusion, although routine screening for atrial fibrillation has not yet become the norm, the management of hypertension generates huge opportunities for opportunistic screening for that arrhythmia, and for mitigating the risk of its occurrence.
I have no conflict of interest
References
(1)Benjamin EJ., Levy D., Vaziri SM et al
Independent risk factors for atrial fibrillation in a population-based cohort: the Framingham Heart Study
JAMA 1994;271:840-844
(2)De Vos CB., Pisters R., Noewlaat R et al
Progression fro paroxysmal to persistent atrial fibrillation. Clinical correlates and prognosis
J Am Coll Cardiol 2010;55:725-731
(3)Soliman EZ., Rahman AKMF., Zhang Z-m et al
Effect of intensive blood pressure lowering on the risk of atrial fibrillation
Hypertension 2020;75:1491-1496

The residual risk of stroke in subjects with nonvalvular atrial fibrillation(NVAF) is, in part, attributable to coexistence of nonvalvular atrial fibrillation(NVAF) and high-grade(stenosis(50% or more severity) involving the intracranial arterial circulation(1). In the latter study concomitant high-grade cerebrovascular stenosis was identified in 231 of 780 consecutive subjects of mean age 69.5 who had undergone angiographic studies at index stroke(1). Coexistence of extracranial carotid artery stenosis(CAS) and NVAF is also a risk factor for residual stroke(2). In the latter study Chang et al identified high-grade CAS(>50% severity) which was ipsilateral to the index ischemic cerebral infarct in 15 out of 25 patients presenting with stroke(2).
Secondary prevention of stroke in NVAF patients who have the association of either high-grade stenotic intracranial cerebrovascular disease or high-grade CAS to which the index stroke can be attributed would entail coprescription of low-dose aspirin and an oral anticoagulant drug. Edoxaban would be a suitable candidate, given the fact that the 15 mg/day dose significantly mitigates the risk of stroke ( of presumably cardioembolic origin) in NVAF subjects aged 80 or more(3). That dose is even lower than the 30 mg/day dose which is associated with significantly(p < 0.001) lower risk of gastrointestinal bleeding than warfarin(4).
Primary prevention would require strict abstinence from smoking, strict control of the lipid profile and strict control of blood pressure.
I have no funding and no conflict of interest.
References
(1) Kim YD., Cha MJ., Kim J et al
Increases in cerebral atherosclerosis according to CHADS2 scores in patients with stroke with nonvalvular atrial fibrillation
STROKE 2011;42:930-934
(2)Chang Y-J., Ryu S-J., Lin S-K
Carotid artery stenosis in ischemic stroke patients with nonvalvuar atrial fibrillation
Cerebrovascular Disease 2002;13:16020
(3)Okumura K., Akao M., Yoshida T et al
Low-dose edoxaban in very elderly patients with atrial fibrillation
N Engl J Med2020;383:1735-1745
(4)Guigliano RP., Ruff CT., Braunwald E et al
Edoxaban versus warfarin in patients with atrial fibrillation
N Engl J Med 2013;369:2093-2104