Научная статья на тему 'Merits of assessing the circadian amplitude and acrophase versus a day-night ratio'

Merits of assessing the circadian amplitude and acrophase versus a day-night ratio Текст научной статьи по специальности «Клиническая медицина»

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Текст научной работы на тему «Merits of assessing the circadian amplitude and acrophase versus a day-night ratio»

Since 1999 ISSN 2226-7417

Электронный научно-образовательный ВЕСТНИК

«Здоровье и образование в XXI веке»

№4 2013 том 15

Dulkova Katarina1, Zeman Michal1, Cornelissen Germaine2, Bada Viliam1, Halberg Franz2, Zaslavskaya Rina M3, Chibisov Sergey M.4 , Kharlickaya Elena V.4, Agarwal R.K.4

(1 Comenius Univ, Bratislava, Slovakia; 2 Univ Minnesota, Minneapolis, MN, USA; 3 Dept of Cardiology, Hospital #60, Moscow, Russia; 4 People's Friendship Univ. of Russia, Moscow, Russia

MERITS OF ASSESSING THE CIRCADIAN AMPLITUDE AND ACROPHASE VERSUS A DAY-NIGHT RATIO.

Some alterations of the circadian pattern of

blood pressure (BP) have been associated with an increased cardiovascular disease risk [1]. Risk assessment is better achieved on the basis of a chronobiological classification relying on the circadian amplitude and acrophase as compared to the conventional day-night ratio (DNR) [2, 3]. Melatonin administration

reportedly restores an altered circadian system [4]. In order to further investigate the relationship between the circadian rhythms in BP and melatonin, we measured endogenous melatonin production in patients treated for conventionally diagnosed hypertension found to have a DNR below or above 10% (‘dippers’ and ‘non-dippers’) [5]. BP was monitored for at least 24 hours with an automatic ambulatory monitor. Plasma melatonin was measured in the middle of the daytime and in the middle of the nighttime by radioimmunoassay. As expected, nocturnal systolic (P<0.05), diastolic (P<0.001) and mean (P<0.001) BP was higher in ‘nondippers’ than in ‘dippers’. No statistically significant difference was found between the

two groups in daytime BP. As expected, mean melatonin concentrations were higher during the night than during the day in both groups. Our earlier analyses showed that for diastolic and mean BP, ‘non-dippers’ had a lower night/day melatonin ratio than ‘dippers’ [5]. Herein, we compare the association of the night/day melatonin ratio with the BP DNR on the one hand and the circadian BP amplitude on the other hand. A statistically significant negative correlation is found between the daytime melatonin concentration and the circadian double amplitude (2A) of systolic (S) BP (r=-

0.266, P=0.042), Figure 1. A statistically

significant positive correlation is found between the nighttime melatonin

concentration and the circadian 2A of heart rate (HR) (r=0.296, P=0.023), Figure 2. A positive correlation is also found between the night/day melatonin ratio and both diastolic (D) BP-2A (r=0.348, P=0.007) and HR-2A (r=0.386,

P=0.003), Figures 3 and 4. By contrast, a similar correlation is not statistically significant in

Электронный научно-образовательный ВЕСТНИК

«Здоровье и образование в XXI веке» №4 2013 том 15

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relation to the DNR of DBP, used to define ‘dipping’ (r=o.ii6, P>o.2o), Figure 5.

Figure 1

Figure 2

The circadian amplitude of melatonin was not determined herein but the two-timepoint approach used for melatonin determination sufficed to show that the association between the circadian variations in BP and melatonin was more readily apparent in relation to the circadian amplitude of BP than to the BP-DNR.

Figure 3

When the circadian rhythm of urinary melatonin excretion is determined, its amplitude correlates with cardiovascular disease risk [6]. Nocturnal melatonin has also been reported to be altered in patients with coronary artery disease [7]. Moreover, melatonin administration in the evening has been shown to lower BP in hypertensive patients, Figure 6, and to improve the

Figure 4

condition of patients with heart failure, Figure 7 [8].

Uncontrolled use of melatonin in hypertensive patients is not warranted, however, as it has been suggested that melatonin may impair the antihypertensive efficacy of calcium channel blockers such as nifedipine [9]. It has also been cautioned that no long- term safety data exist for the continued use of melatonin, and the

Электронный научно-образовательный ВЕСТНИК

«Здоровье и образование в XXI веке» №4 2013 том 15

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optimal dose and formulation for any application remains to be clarified [10]. Timing should also be kept in mind both from the viewpoint of optimizing efficacy but also from that of minimizing undesirable effects in view of the involvement of melatonin in feedsidewards [11-13].

1. Halberg F, Cornelissen G, Halberg J, Fink

H, Chen C-H, Otsuka K, Watanabe Y, Kumagai

Y, Syutkina EV, Kawasaki T, Uezono K, Zhao ZY, Schwartzkopff O. Circadian Hyper-Amplitude-Tension, CHAT: a disease risk

syndrome of anti-aging medicine. J Anti-Aging Med 1998; 1: 239-259.

2. Otsuka K, Cornelissen G, Halberg F. Predictive value of blood pressure dipping and swinging with regard to vascular disease risk. Clinical Drug Investigation 1996; 11: 20-31.

3. Bingham C, Cornelissen G, Chen C-H, Halberg F. Chronobiology works when day-night ratios fail in assessing cardiovascular disease risk from blood pressure profiles. Abstract, III International Conference, Civilization diseases in the spirit of V.I. Vernadsky, People's Friendship University of Russia, Moscow, Oct. 10-12, 2005, p. 111-113.

4. Sack RL, Lewy AJ. Melatonin as a

chronobiotic: treatment of circadian

desynchrony in night workers and the blind. J Biological Rhythms 1997; 12: 595-603.

5. Zeman M, Dulkova K, Bada V, Herichova

I. Plasma melatonin concentrations in hypertensive patients with the dipping and non-dipping blood pressure profile. Life

^j] Sciences 2005; 76: 1795-1803.

<^=0 6. Wetterberg L, Halberg F, Halberg E, Haus

E, Kawasaki T, Ueno M, Uezono K, Cornelissen G, Matsuoka M, Omae T. Circadian characteristics of urinary melatonin from clinically healthy women at different civilization disease risk - Acta med scand 1986; 220: 71-81.

7. Yaprak M, Altun A, Vardar A, Aktoz M, Ciftci S, Ozbay G. Decreased nocturnal synthesis of melatonin in patients with coronary artery disease. Int J Cardiol 2003; 89: 103-107.

8. Zaslavskaya RM, Lilitsa GV,

Dilmagambetova GS, Halberg F, Cornelissen G, Otsuka K, Singh RB, Stoynev A, Ikonomov O, Tarquini R, Perfetto F, Schwartzkopff O, Bakken EE. Melatonin, refractory hypertension, myocardial ischemia and other challenges in nightly blood pressure lowering. Biomed & Pharmacother 2004; 58 (Suppl 1): S129-S134.

9. Lusardi P, Piazza E, Fogari R.

Cardiovascular effects of melatonin in

hypertensive patients well controlled bynifedipine: a 24-hour study. Brit J Clin

Pharmacol 2000; 49: 423-427.

10. Arendt J, Skene DJ. Melatonin as a chronobiotic. Sleep Medicine Reviews 2005; 9:

25-39-

11. Sanchez de la Pena S. The feedsideward of cephalo-adrenal immune interactions.

Chronobiologia 1993; 20: 1-52.

12. Cornelissen G, Halberg F, Perfetto F, Tarquini R, Maggioni C, Wetterberg L.

Melatonin involvement in cancer: methodological considerations. In: Bartsch C, Bartsch H, Blask DE, Cardinali DP, Hrushesky WJM, Mecke W (eds). The Pineal Gland and Cancer: Neuroimmunoendocrine Mechanisms

Электронный научно-образовательный ВЕСТНИК

«Здоровье и образование в XXI веке» №4 2013 том 15

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i n Malignancy. Heidelberg: Springer; 2001. p.

117-149.

13. Halberg F, Cornelissen G, Katinas GS,

Watanabe Y, Otsuka K, Maggioni C, Perfetto F,

Tarquini R, Schwartzkopff O, Bakken EE.

Feedsidewards: intermodulation (strictly)

among time structures, chronomes, in and around us, and cosmo- vasculo-neuroimmunity. About ten-yearly changes: what Galileo missed and Schwabe found. Ann NYAS 2000; 917: 348-376.

Acknowled gement: This work was supported by grants APVT-20-022704 (MZ) & GM-13981 (FH).

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