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Cycling above rather than below lactate threshold is more effective for nitric oxide release and post-exercise blood pressure reduction in individuals with type-2 diabetes

Ciclismo arriba del umbral de lactato es más efectivo que abajo para la liberación de óxido nítrico y reducción de la presión arterial después del ejercicio en individuos con diabetes tipo 2

Ciclismo acima do limiar de lactato é mais efetivo que abaixo para liberação de óxido nítrico e redução da pressão arterial pós-exercício em indivíduos com diabetes tipo 2

Abstracts

The purposes of this study were to analyze and compare the effects of exercise performed in different intensities, above and below lactate threshold (LT) on post-exercise blood pressure (BP) and nitric oxide (NO) responses in individuals with type 2 diabetes (T2D). For this, 11 T2D underwent the following sessions: 1) control session; 2) 20-min of moderate cycling (80% LT); and 3) 20-min of high intensity cycling (120%LT) on a cycle ergometer. Plasma NO and BP measurements were carried out at rest and at 15 and 45 min of post-sessions. When compared to rest, only the exercise session performed at 120%LT elicited an increase of NO (from 7.2 to 9.5 µM, p<0.05), as well as a decrease in systolic BP (from 126.6±7.9 to 118.7±3.9 mmHg, p<0.05) during the post-exercise period. In conclusion, the results suggest that NO release and post-exercise BP decrease are intensity-dependent for individuals with T2D.

nitric oxide; type-2 diabetes; high intensity exercise


Los objetivos del presente estudio fueron examinar y comparar los efectos del ejercicio realizado en diferentes intensidades, arriba y abajo del umbral de lactato (UL), sobre la respuesta de la presión arterial (PA) y el óxido nítrico (NO) en individuos con diabetes tipo 2 (DM2). Por lo tanto, 11 DM2 se sometieron las siguientes sesiones: 1) sesión control; 2) 20 min de ejercicio en cicloergómetro a una intensidad moderada (80%UL); y 3) 20 min de ejercicio en cicloergómetro a una intensidad alta (120%UL). El NO plasmático y las mediciones de la PA fueron realizados en reposo y en 15 y 45 min del período de recuperación para todas las sesiones. En comparación con el período de reposo, sólo la sesión de ejercicio realizado a 120%UL promovió aumento de NO (7,2 para 9,5 µM, p<0,05) y, por lo tanto, una disminución de la presión arterial sistólica (de 126,6±7,9 para 118,7±3,9 mmHg, p<0,05) durante el período de recuperación después del ejercicio. En conclusión, los resultados sugieren que la liberación de NO y la disminución de PA parece ser intensidad-dependiente para individuos con DM2.

óxido nítrico; diabetes tipo 2; ejercicio de alta intensidad


Os objetivos do presente estudo foram analisar e comparar os efeitos do exercício realizado em diferentes intensidades, acima e abaixo do limiar de lactato (LL), sobre a resposta da pressão arterial (PA) e óxido nítrico (NO) em indivíduos com diabetes tipo 2 (DM2). Para tanto, 11 DM2 foram submetidos às seguintes sessões: 1) sessão controle; 2) 20 min de exercício em cicloergômetro em intensidade moderada (80%LL); e 3) 20 min de exercício em cicloergômetro em alta intensidade (120%LL). O NO plasmático e as medidas de PA foram realizadas no repouso, bem como aos 15 e 45 min do período de recuperação de todas as sessões. Quando comparado ao período de repouso, somente a sessão de exercício realizado a 120%LL promoveu aumento do NO (de 7,2 para 9,5 µM, p<0,05) e, por conseguinte, uma diminuição na pressão arterial sistólica (de 126,6±7,9 para 118,7±3,9 mmHg, p<0,05) durante o período de recuperação pós-exercício. Em conclusão, os resultados sugerem que a liberação de NO e a diminuição da PA parecem ser intensidade-dependente para indivíduos com DM2.

óxido nítrico; diabetes tipo 2; exercício de alta intensidade


ORIGINAL ARTICLE

Cycling above rather than below lactate threshold is more effective for nitric oxide release and post-exercise blood pressure reduction in individuals with type-2 diabetes

Ciclismo acima do limiar de lactato é mais efetivo que abaixo para liberação de óxido nítrico e redução

da pressão arterial pós-exercício em indivíduos com diabetes tipo 2

Ciclismo arriba del umbral de lactato es más efectivo que abajo para la liberación de óxido nítrico y

reducción de la presión arterial después del ejercicio en individuos con diabetes tipo 2

Ricardo Yukio AsanoI; Rodrigo Alberto Vieira BrowneII; Rafael da Costa SoteroIII; Marcelo Magalhães SalesIII; José Fernando Vila Nova de MoraesIII; Carmen Sílvia Grubert CampbellIII; Herbert Gustavo SimõesIII

ICatholic University of Brasília, Brazil

IIFederal University of Rio Grande do Norte, Brazil

IIICatholic University of Brasília, Brazil

Correspondence Correspondence: Ricardo Yukio Asano and Herbert G Simões Programa de Pós-Graduação Stricto Sensu em Educação Física da Universidade Católica de Brasília EPTC, QS 07, LT 1, BL G, Sala 116 Águas Claras, Brasília 72.022-900 DF, Brasil Phone: +55 (11) 97011-5500 Email: ricardokiu@ig.com.br; hgsimoes@gmail.com

ABSTRACT

The purposes of this study were to analyze and compare the effects of exercise performed in different intensities, above and below lactate threshold (LT) on post-exercise blood pressure (BP) and nitric oxide (NO) responses in individuals with type 2 diabetes (T2D). For this, 11 T2D underwent the following sessions: 1) control session; 2) 20-min of moderate cycling (80% LT); and 3) 20-min of high intensity cycling (120%LT) on a cycle ergometer. Plasma NO and BP measurements were carried out at rest and at 15 and 45 min of post-sessions. When compared to rest, only the exercise session performed at 120%LT elicited an increase of NO (from 7.2 to 9.5 µM, p<0.05), as well as a decrease in systolic BP (from 126.6±7.9 to 118.7±3.9 mmHg, p<0.05) during the post-exercise period. In conclusion, the results suggest that NO release and post-exercise BP decrease are intensity-dependent for individuals with T2D.

Keywords: nitric oxide, type-2 diabetes, high intensity exercise

RESUMO

Os objetivos do presente estudo foram analisar e comparar os efeitos do exercício realizado em diferentes intensidades, acima e abaixo do limiar de lactato (LL), sobre a resposta da pressão arterial (PA) e óxido nítrico (NO) em indivíduos com diabetes tipo 2 (DM2). Para tanto, 11 DM2 foram submetidos às seguintes sessões: 1) sessão controle; 2) 20 min de exercício em cicloergômetro em intensidade moderada (80%LL); e 3) 20 min de exercício em cicloergômetro em alta intensidade (120%LL). O NO plasmático e as medidas de PA foram realizadas no repouso, bem como aos 15 e 45 min do período de recuperação de todas as sessões. Quando comparado ao período de repouso, somente a sessão de exercício realizado a 120%LL promoveu aumento do NO (de 7,2 para 9,5 µM, p<0,05) e, por conseguinte, uma diminuição na pressão arterial sistólica (de 126,6±7,9 para 118,7±3,9 mmHg, p<0,05) durante o período de recuperação pós-exercício. Em conclusão, os resultados sugerem que a liberação de NO e a diminuição da PA parecem ser intensidade-dependente para indivíduos com DM2.

Palavras-chave: óxido nítrico, diabetes tipo 2, exercício de alta intensidade

RESUMEN

Los objetivos del presente estudio fueron examinar y comparar los efectos del ejercicio realizado en diferentes intensidades, arriba y abajo del umbral de lactato (UL), sobre la respuesta de la presión arterial (PA) y el óxido nítrico (NO) en individuos con diabetes tipo 2 (DM2). Por lo tanto, 11 DM2 se sometieron las siguientes sesiones: 1) sesión control; 2) 20 min de ejercicio en cicloergómetro a una intensidad moderada (80%UL); y 3) 20 min de ejercicio en cicloergómetro a una intensidad alta (120%UL). El NO plasmático y las mediciones de la PA fueron realizados en reposo y en 15 y 45 min del período de recuperación para todas las sesiones. En comparación con el período de reposo, sólo la sesión de ejercicio realizado a 120%UL promovió aumento de NO (7,2 para 9,5 µM, p<0,05) y, por lo tanto, una disminución de la presión arterial sistólica (de 126,6±7,9 para 118,7±3,9 mmHg, p<0,05) durante el período de recuperación después del ejercicio. En conclusión, los resultados sugieren que la liberación de NO y la disminución de PA parece ser intensidad-dependiente para individuos con DM2.

Palabras clave: óxido nítrico, diabetes tipo 2, ejercicio de alta intensidad

Introduction

Type-2 diabetes (T2D) is among the diseases with higher incidence and prevalence throughout the world (Wild, Roglic, Green, Sicree, & King, 2004), and is associated mainly with a sedentary lifestyle and inadequate feeding habits (Hu et al., 2001). This pathology is associated to several cardiovascular complications, including endothelial dysfunction and arterial hypertension (Resnick & Howard, 2002). Endothelial dysfun-ction results in a lower activity of vasodilator proteins such as those of kallikrein-kinin system, and therefore in a lower bioavailability of endothelial nitric oxide (NO) (Miche et al., 2006).

Physical exercise has been recommended as a non-pharmacological treatment of systemic arterial hypertension (SHA) (Chobanian et al., 2003) and T2D (Colberg et al., 2010), since it elicits a significant post-exercise blood pressure (BP) and glycaemia reduction. The lactate threshold (LT) has been applied on aerobic evaluation and exercise prescription for individuals with T2D (Sales et al., 2012; Morais et al., 2011; Motta et al., 2010), once exercise below LT is considered a safe intensity associated to a low metabolic and cardio-vascular stress (Sales et al., 2011; Simões, Moreira, Moffatt, & Campbell, 2010). On the other hand, the benefits of exercise may be dependent of which intensity it is performed (Bahr & Sejersted, 1991).

Some studies revealed that a single exercise session can promote a significant BP decrease over minutes or hours after exercise, when compared to pre-exercise values (Sales et al., 2012; Morais et al., 2011; Motta et al., 2010; Simões, Moreira, Moffatt, & Campbell, 2010). This phenomenon is known as post-exercise hypotension (PEH) and has been suggested to be dependent of NO release, which is a powerful vasodilator (Asano et al., 2012; Santana et al., 2011; Patil, DiCarlo, & Collins, 1993). However the mechanisms and the relationships between NO release and PEH remain inconclusive (Halliwill, Minson, & Joyner, 2000; Pescatello, Fargo, Leach, & Scherzer, 1991), especially for T2D .

On the other hand, previous studies have suggested that, after performing exercise around the LT intensity, individuals with T2D present lower post-exercise BP reduction when compared to their non-diabetic (ND) pairs (Motta et al., 2010; Lima et al., 2008). This could be partially explained by the decreased activity of plasma kallikrein (Motta et al., 2010), as well as a lower NO release in this population (Asano et al., 2012; Stabler, Katherine, Ham, Jelesoff, & Allen, 2010).

The effects of different exercise intensities on both NO release and PEH in individuals with T2D are still unknown. The present study hypothesized that both NO production and the occurrence of PEH, in individuals with T2D, would be dependent of exercise intensity domain. Thus, exercise performed above LT would elicit a higher NO release and a more significant PEH in individuals in T2D due to a higher metabolic and cardiovascular stress (Moreira, Simões, Hiyane, Campbell, & Simões, 2007; Simões et al., 2010). Therefore, the aim of the present study was to analyze and compare the effects of different exercise intensities (above and below LT) on post-exercise BP and NO responses for individuals with T2D.

Method

Sample

After approval from the ethics committee of the Catholic University of Brasília (n. 167/2011) and signature of the informed consent form, eleven individuals clinically diagnosed with type-2 diabetes, from both sexes, and non-smokers, were evaluated (Table 1). Though non-insulin dependent, the volunteers were taking oral hypoglycemiants such as sulfonylureas, metformin, metformin+glibenclamide, glimepiride, pioglitazone chloridrate and/or had controlled food intake. Exclusion criteria for participation included detection of any abnormality in the resting electro-cardiogram observed by a cardiologist, previous diagnosis of peripheral and autonomic neuropathy, retinopathy, as well as diabetic foot ulcerations, orthopedic complications, or any other problems that could impair the participants' ability to complete all the study procedures. Participants under use of insulin were not included in the studied sample.

Procedures

Two hours before all experimental sessions the volunteers ingested a standard breakfast with a moderate glycaemic index. The 'breakfast kit' was composed by a 40 g vanilla flavoured mini-cake (Pullman®), a 200 ml cup of mango flavoured light juice (Minute Maid Plus®) and a 30 g salty biscuit pack (Pit Stop®). In total, 315 kcal were offered from 51.6 g of carbohydrate (66.9%), 4.6 g of protein (5.8%) and 9.5 g of fat (27.1%). The glycaemic index of the 'kit' was considered moderate.

The volunteers were instructed to interrupt the use of medicines (time to partially offset the effects of medicaments, and prevent damage to blood glucose and blood pressure of volunteers), to refrain from physical activity and to avoid ingestion of alcoholic beverages and caffeine during the 24 hours that preceded experimental sessions.

Throughout the study, the volunteers visited the Physical Evaluation and Training Laboratory at the Catholic University of Brasília four times. The first visit consisted of a maximal incremental test on a cycle ergometer in order to determine LT. Afterwards, the subjects underwent to three sessions: exercise at moderate intensity (80% LT); high intensity (120% LT), and a control session (without exercise). The intensities were classified as moderate (below LT) and intense (above LT) according to previous authors Poole and Richardson (1997), Simões, Denadai, Baldissera, Campbell, and Hill (2005) and Denadai and Caputo (2003). Experimental sessions were performed in a randomized order, with an interval that varied from 72 to 120 hours between experimental sessions.

Incremental exercise test

Initially, the volunteers remained seated for 20 min and then a resting electrocardiogram was performed and blood glucose was measured. Afterwards, an incremental test using an electromagnetic cycle ergometer (Lode Excalibur Sport, Netherlands) was initiated. The test started with a 1-minute warm-up at 60 rpm without load, followed by a 15-watt increment at each 3-minute stage until volitional exhaustion.

During rest before exercise, as well as during the last 10 seconds of each incremental stage, 25 µL of blood were collected from earlobe. These blood samples were collected after puncture by using disposable lancets and heparinized capillary tubes (the first drop of blood was discharged to prevent sample contamination). The blood samples were then stored in microtubes (Eppendorf®) containing 50µL of sodium fluoride (NaF) at 1% for later analysis of lactate concentra-tions [Lac] through the electroenzymatic method (Yellow Springs 2700S).

Expired gases were measured during the incremental test through a gas analyzer (Metalyzer 3B, Cortex Biophysik, Germany), which was previously calibrated with a 3L syringe (flow calibration) and a mixed pattern of gas containing 4.9% of CO2 and 17.0% of O2 (gas calibration). The values of ventilation (VE), oxygen consumption (VO2), and carbon dioxide production (VCO2) were registered during the last 20 sec of each 3 min stage. In addition, BP (Microlife®) and heart rate (HR) (Polar S810, Kempele, Finland) were also measured. VO2 peak was considered as the highest oxygen consumption attained at the exhaustion moment (Howley, Bassett, & Welch, 1995). Electrocardiograph patterns were registered and accompanied by a cardiologist throughout the whole test.

Lactate threshold determination (LL)

In order to determine LL, the [Lac] kinetics during the incremental test was analyzed. The exercise intensity (Watts) corresponding to the LL was determined by visual inspection, by considering the exercise intensity in which an over proportional increase of [Lac] was observed (Sales et al., 2011). In addition, whenever necessary the second order polynomial function, which consist of applyind the [Lac] workload ratio versus increase workload to identify the vertices and thus confirm the LL intensity (Simões, Moreira, Moffatt, & Campbell, 2010).

120% LT session (S120)

The S120 was considered a high intensity exercise session and consisted of 20 min of aerobic exercise on a cycle ergometer (Lode Excalibur Sport, Netherlands) at a constant load corresponding to 120% of the LT.

80% LT session (S80)

The S80 session was considered moderate exercise session and consisted of a 20 min cycle ergometer exercise (Lode Excalibur Sport, Netherlands) at a constant load corresponding to 80% of the LT.

Control session (CON)

During the CON session, participants remained at rest in a seated position for 20 min without exercise. However, the same data collection procedures were carried out, as described in the S120 and S80 session.

Pre- and post-exercise procedures

Prior to the S120, S80 and CON sessions, the participants remained seated at rest for blood sampling, as well as for collection of hemodynamic and respiratory variables. The measured variables included BP (BP 3AC1-1, Microlife AG, Widnau, Switzerland), HR (Polar® S810i, Polar Electro Oy Kempele), as well as blood lactate [Lac] and glucose (bGluc) (YSI 2700, YSI Inc, Yellow Springs, OH, USA). The 25 µL of blood were collected from ear lobe following the same procedures described in the incremental test section. The pre-exercise measures were done every 5 min up to 20 min. The BP and HR were measured at the same moments. After performing exercise and CON, the volunteers remained seated for 45 min in which capillary blood (25 µL) and venous blood (8 ml) were collected at the 15th and 45th min of post exercise recovery period.

Venous blood sample collection

Blood samples (8 ml) were collected for NO analysis using a hypodermic syringe and deposited in two vacuette® tubes (4 ml) (BD, New Jersey, USA) containing EDTA. The samples were centrifuged at room temperature for 15 min at 3000 rpm. The plasma aliquots were separated in microtubes (Eppendorf®) and immediately stored at -20ºC.

Nitric oxide (NO) concentration

Plasma NO concentration was predicted from plasma nitrite measurements. For this 50µL of phosphate-buffered saline (PBS) were added in the sample's standard curve wells using 96-well plates. Afterwards, 100µL of NaNO2 at 100µM, previously diluted in a 1:200 ratio, were added in the first sample's standard curve wells. Later, successive dilutions in a 1:2 ratio in the following wells were performed to determine the nitrite's standard curve. In the sample's wells, 50µL of plasma were added together with 100µL of a mixture containing sulfanilide at 1.0% in phosphoric acid at 2.5%, and naftiletilenodiamide at 1.0% in phosphoric acid at 2.5% in a 1:1 ratio was added. After 10 min of incubation at room temperature the ELISA reading at 540 nm was performed. The amount of nitrite from each sample was calculated using the absorbance linear regression equation from the known quantity of nitrite from the NaNO2 solution (200µM to 0.097µM) (Tsikas, 2007).

Statistical analysis

Normality of data was tested through skewness and kurtosis tests, with all variables presenting values between -1.0 and + 1.0. Analysis of variance (ANOVA) for repeated measures with Bonferroni's post hoc were applied to compare between (S120, S80 and CON) and within (rest, 15 min post-exercise, and 45 min post-exercise) values of systolic blood pressure, diastolic blood pressure, mean blood pressure and nitrite (as NO measure). Pearson correlation was applied between NO results and PEH. Data are expressed in mean ± standard deviation. The level of significance adopted was 5% (p<0.05) and all procedures were performed using the Statistical Package for the Social Sciences (SPSS) v.15.0 for windows.

Results

Table 1 presents the main characteristics of the sample regarding anthropometry, body composition, fasting glucose and BP.

The results from the present study indicate that the chosen exercise intensities were significantly distinct, since VO2 at S120 was higher than S80 (17.6±0.8 vs. 13.4±0.3 ml.kg-1.min-1, p<0.05), and both sessions presented significantly higher mean oxygen uptake when compared to CON (2.9±0.1 ml.kg-1.min-1, p<0.05), as shown in Figure 1. Table 2 presents the percentage of maximal oxygen uptake (VO2max) in which exercise was performed and the rate pressure product as a marker of cardiovascular stress.


Regarding the NO, only the S120 session elicited a significant increase of this variable after exercise (from 7.2 µM to 9.5 µM, p<0.05) (Figure 2).


Post-exercise systolic blood pressure (SBP) decreased significantly (p<0.05) at the 15th and 45th min of S120 when compared to pre-exercise resting values. In addition, only this session elicited a significantly lower SBP values when compared to CON. Diastolic blood pressure (DBP) and mean arterial pressure (MAP) showed no significant changes after exercise during the experimental sessions (Table 3).

The correlation between NO and SBP after exercise session at 120% LT (S120) showed a moderate and significant (p<0.05) correlation coefficient (r=0.55) (Figure 3).


Discussion

The main findings of the present study were that exercise performed at a higher intensity (120% of LT) promoted an increase in NO production and, consequently, post-exercise BP reduction in individuals with T2D. On the other hand, such findings were not evidenced when exercise was performed at a moderate intensity (80% of LT), since no significant changes were shown in both NO and post-exercise BP. In this scenario, exercise performed in a higher exercise intensity domain seemed to favor a better post-exercise BP control for individuals with T2D. But the correlation between NO and PEH was only moderate.

Similar results have been found in a recent study from our laboratory (Santana et al., 2011) in which a significant increase in salivary NO and greater PEH were observed after high intensity exercise in elderly women.

In the present study the moderate intensity exercise session was not able to promote an increase in NO production and, therefore, no PEH was presented by our participants. Corroborating to this, Motta et al. (2010), while investigating the effect of T2D on post-exercise of plasma kallikrein activity (a precursor of NO production) and BP after moderate exercise (90% of LT), found a significant increase in plasma kallikrein activity and reduction of BP in non-diabetic subjects but not in individuals with T2D. Thus, it is possible that individuals with T2D would be benefitted from exercise bouts performed at higher intensities. Likewise, Lima et al. (2008) found a PEH of greater magnitude and duration in individuals with T2D after performing exercise at 110% LT when compared to 90% LT. However, in these last studies (Motta et al., 2010; Lima et al., 2008), NO was not measured.

In the present study the production of NO seemed to be also dependent of the intensity in which exercise was performed, since only the S120 resulted in a significant increase in NO concentration associated to a decreased SBP during the post-exercise recovery period. Santana et al. (2011), while investigating the effects of different exercise intensities (maximal exercise vs. 90% LT intensity) on NO release and post-exercise BP in elderly individuals, also demonstrated a significant NO increase together with PEH only when the higher intense exercise was performed.

T2D is associated with a decreased activity of the kallikrein-kinin system and elevated oxidative stress that may elicit endothelial dysfunction (Sharma & Narayanan, 2011; Rodrigo et al., 2007). These processes result in a lower NO release and thus a decreased vasodilation (Asano et al., 2012; Stabler, Katherine, Ham, Jelesoff, & Allen, 2010). Therefore, these factors could partially explain the impaired ability that individuals with T2D have to present PEH, especially when exercise is performed at lower intensities. However, the effects of performing exercise in different intensities (eg. moderate vs. intense) and type of intervention (i.e. chronic vs. acute exercise) on the endothelial function of individuals with T2D need further investigation.

In spite of this, a moderate correlation between NO release and PEH was observed in the present study, suggesting a possible relationship between exercise intensity, NO release and PEH. Investigations with animal models have suggested that the occurrence of PEH may be mediated by NO (Howard & DiCarlo, 1992; Patil, DiCarlo & Collins, 1993). However, the relationship between these factors and mechanisms in humans remain inconclusive. Kingwell, Formosa, Muhlmann, Bradley and McConell (2002) found that the persistent peripheral vasodilation after a single bout of moderate-intensity exercise is resistant to nitric oxide synthase inhibition, and it does not appear that PEH would be dependent of increased production of NO in young healthy humans. To our knowledge, however, the present investigation is the first study in humans with T2D analyzing the effects of exercise at different domains of intensity (e.g. below LT = moderate vs. above LT = intense) on both NO and PEH.

In order to benefit from PEH, the T2D individuals with controlled BP and glucose should perform exercise slightly above the anaerobic threshold. These benefits would probably occur due to the higher metabolic and mechanical stress promoted by exercise at such intensity (Teodoro, Natali, Fernandes & Peluzio, 2010), since PEH is dependent of exercise intensity induced by the increase of the activity of the kallikrein-kinin system, and in consequence, a higher NO release (Pontes et al., 2008). Pharmacological treatments that increase the activity of the kallikrein-kinin system, and thus the production of NO, have shown efficacy in the treatment of individuals with hypertension and T2D (Moreira, Simões, Hiyane, Campbell, & Simões, 2007). On the other hand, non-pharmacological treatments, such as exercise, have also been characterized as good strategy to improve endothelial function (Rallidis et al., 2009), especially for not presenting collateral effects. Furthermore, Kingwell, Formosa, Muhlmann, Bradley, & McConell (2002) demons-trated a strong association between glucose uptake and NO production during exercise in T2D.

Even though individuals with type-2 diabetes have impaired NO production at rest (Ghosh, Sherpa, Bhutia, Pal, & Dahal, 2011), aerobic exercise seems to acutely increase the production of this metabolite in T2D population, especially in more intense exercise sessions. Additionally, studies have also associated a higher production of NO in T2D individuals with an increase in glucose uptake (Kingwell, Formosa, Muhlmann, Bradley, & McConell, 2002; Mcconell & Kingwell, 2006), both effects being extremely relevant for T2D.

Moreover, the 120% LT session was considered safe for our participants, once the main cardiovascular, metabolic and ventilatory responses did not increase over proportionally during exercise session, remaining within recommended values (American College of Sports Medicine, 1998). On the other hand, we suggest caution on prescribing aerobic exercise above LT, particularly in sessions lasting up to 20 minutes for individuals with low fitness and clinical limitations to exercise. If applicable, prescription of high intensity exercise should be done on an individual basis (e.g. severity of diabetes should be considered) and after appropriate medical screening. Such above LT prescriptions should be limited to those patients without cardiovascular and metabolic complications.

One possible limitation of the present study was the absence of a control group of individuals without diabetes. However, previous studies have already presented that individuals with T2D have lower production of NO, lower vasodilation, and, consequently, higher BP values at rest when compared to their non-diabetic pairs (Mather, Lteif, Steinberg, & Baron, 2004). Moreover, the intensities of the session were different (120% LL and 80% LL) but the exercise duration was the same (20 minutes) for both sessions. Thus, the training load was higher during the intense exercise session (S120). Therefore, it is important that future studies comparing exercise performed in the same workload but in different intensities in order to evaluate the differences related to intensity and training load.

Conclusion

Based on the present findings, we conclude that NO production and the occurrence of PEH seems to be dependent of exercise intensity, since only exercise performed above the LT significantly increased the production of NO and promoted PEH in individuals with T2D. However, the prescription of high intensity exercise must be done with caution and on an individual basis. Therefore, future research on this topic should focus on the safety of exercise protocols above the LT, as well as the chronic effects of exercise on the production of NO and PEH in individuals with diabetes.

Authors' note

Ricardo Yukio Asano is affiliated with the Catholic University of Brasília, Brasília, Distrito Federal, Brazil and the Municipal foundation of higher education in Bragança Paulista - Brazil.

Rodrigo Alberto Vieira Browne is affiliated with the Federal University of Rio Grande do Norte, Natal, Rio Grande do Norte, Brazil;

Rafael da Costa Sotero, Marcelo Magalhães Sales, Carmen Sílvia Grubert Campbell1and Herbert Gustavo Simões are affiliated with the Catholic University of Brasília, Brasília, Distrito Federal, Brazil;

José Fernando Vila Nova de Moraes is affiliated with the Catholic University of Brasília, Brasília, Distrito Federal, Brazil and the Federal University of Vale do São Francisco, Petrolina, Pernambuco, Brazil.

Funding

This work was supported by the Conselho Nacional de Desenvolvimento Científico e Tecnológico - CNPq/Universal [grant number 473598/2010-8] and Coordenação de Aperfeiçoamento de pessoal de nível superior (CAPES/PROCAD-NF).

Acknowledgements

The authors would like to thank to the Coordenação de Aperfeiçoa-mento de Pessoal de Nível Superior (CAPES) and Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq) for the finantial support to the study, as well as for the Master's scholarship grants (CAPES), PhD (CAPES and CNPq), and for an independent research grant (CNPq).

Manuscript received on March 30, 2013

Manuscript accepted on May 17, 2013

Declaration of Conflicting Interests: The authors declared no conflicts of interest exist with respect to the research, authorship, and/or publication of this article.

This study was presented at the 8th International Congress of Physical Education and Human Movement and 14th Symposium Paulista Physical Education.

  • American College of Sports Medicine. (1998). Exercise for patients with coronary artery disease. Medicine and Science in Sports and Exercise, 5, 1-5.
  • Asano, R. Y., Sales, M. M., Coelho, J. M., Moraes, J. F. V. N., Pereira, L. A., Campbell, C. S. G., & Simões, H. G. (2012). Exercise, nitric oxide, and endothelial dysfunction: a brief review. Journal of Exercise Physiology Online, 15, 76-86.
  • Bahr, R., & Sejersted, O.M. (1991). Effect of intensity of exercise on excess postexercise O2 consumption. Metabolism: Clinical and Experimental, 40, 836-841.
  • Chobanian, A. V., Bakris, G. L., Black, H. R., Cushman, W. C., Green, L. A., Izzo J. L. Jr., ... National High Blood Pressure Education Program Coordinating Committee. (2003). The National High Blood Pressure Education Program Coordinating Committee: the seventh report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure: the JNC 7 report. JAMA: The Journal of the American Medical Association, 289, 2560-2572.
  • Colberg, S. R., Sigal, R. J., Fernhall, B., Regensteiner, J. G., Blissmer, B. J., Rubin, R. R., ... American Diabetes Association. (2010). Exercise and type 2 diabetes: the American College of Sports Medicine and the American Diabetes Association: joint position statement. Diabetes Care, 33, 147-167.
  • Denadai, B. S., & Caputo, F. (2003). Efeitos do treinamento sobre a cinética do consumo de oxigênio durante o exercício realizado nos diferentes domínios de intensidade de esforço. Motriz, 9, S1-S7.
  • Ghosh, A., Sherpa, M. L., Bhutia, Y., Pal, R., & Dahal, S. (2011). Serum nitric oxide status in patients with type 2 diabetes mellitus in Sikkin. International Journal of Applied and Basic Medical Research, 1, 31-35.
  • Halliwill, J. R., Minson, C. T., & Joyner, M. J. (2000). Effect of systemic nitric oxide synthase inhibition on postexercise hypotension in humans. Journal of Applied Physiology, 89, 1830-1836.
  • Howard, M. G. & DiCarlo, S. E. (1992). Reduced vascular responsiveness after a single bout of dynamic exercise in the conscious rabbit. Journal of Applied Physiology, 73, 2662-2667.
  • Howley, E., Bassett, D. J., & Welch, H. (1995). Criteria for maximal oxygen uptake: review and commentary. Medicine and Science in Sports and Exercise, 27, 1292-1301.
  • Hu, F. B., Leitzmann, M. F., Stampfer, M. J., Colditz, G. A., Willett, W. C., & Rimm, E. B. (2001). Physical activity and television watching in relation to risk for type 2 diabetes mellitus in men. Archives of Internal Medicine, 161, 1542-1548.
  • Kingwell, B. A., Formosa, M., Muhlmann, M., Bradley, S. J., & McConell, G. K. (2002). Nitric oxide synthase inhibition reduces glucose uptake during exercise in individuals with type 2 diabetes more than in control subjects. Diabetes, 51, 2572-2580.
  • Lima, L. C., Assis, G. V., Hiyane, W., Almeida, W. S., Arsa, G., Baldissera, V., ... Simões, H. G. (2008). Hypotensive effects of exercise performed around anaerobic threshold in type 2 diabetic patients. Diabetes Research and Clinical Practice, 81, 216-222.
  • Mather, K. J., Lteif, A., Steinberg, H. O., & Baron, A. D. (2004). Interactions between endothelin and nitric oxide in the regulation of vascular tone in obesity and diabetes. Diabetes, 53, 2060-2066.
  • Mcconell, G. K., & Kingwell, B. A. (2006). Does nitric oxide regulate skeletal muscle glucose uptake during exercise? Exercise and Sport Sciences Reviews, 34, 36-41.
  • Miche, E., Herrmann, G., Nowak, M., Wirtz, U., Tietz, M., Hürst, M., ... Radzewitz, A. (2006). Effect of an exercise training program on endothelial dysfunction in diabetic and non-diabetic patients with severe chronic heart failure. Clinical Research in Cardiology, 95, 117-124.
  • Morais, P. K., Campbell, C. S. G., Sales, M. M., Motta, D. F., Moreira, S. R., Cunha, V. N. C., ... Simões, H. G. (2011). Acute resistance exercise is more effective than aerobic exercise for 24 h blood pressure control in type 2 diabetics. Diabetes & Metabolism, 37, 112-117.
  • Moreira, S. R., Simões, G. C., Hiyane, W. C, Campbell, C. S. G., & Simões, H. G. (2007). Identificação do limiar anaeróbio em indivíduos com diabetes tipo-2 sedentários e fisicamente ativos. Revista Brasileira de Fisioterapia, 11, 289-296.
  • Motta, D. F., Lima, L. C. J., Arsa, G., Russo, P. S., Sales, M. M., Moreira, S. R., ... Campbell, C. S. G. (2010). Influence of type 2 diabetes on kallikrein activity after physical exercise and its relationship with post exercise hypotension. Diabetes & Metabolism, 36, 363-368.
  • Patil, R. D., DiCarlo, S. E. & Collins, H. L. (1993). Acute exercise enhances nitric oxide modulation of vascular response to phenylephrine. American journal of physiology. Heart and circulatory physiology, 265, 184-188.
  • Pescatello, L. S., Fargo, A. E., Leach, C. N. Jr, & Scherzer H. H. (1991). Short-term effect of dynamic exercise on arterial blood pressure. Circulation, 83, 1557-1561.
  • Pontes, F. L. Jr, Bacurau, R. F., Moraes, M. R., Navarro, F., Casarini, D. E., Pesquero, J. L., ... Piçarro, I. C. (2008). Kallikrein kinin system activation in postexercise hypotension in water running of hypertensive volunteers. International Immunopharmacology, 8, 261-266.
  • Poole, D. C., & Richardson, R. S. (1997). Determinants of oxygen uptake. Implications for exercise testing. Sports Medicine, 24, 308-320.
  • Rallidis, L. S., Lekakis, J., Kolomvotsou, A., Zampelas, A., Vamvakou, G., Efstathiou, S., ... Kremastinos, D. T. (2009). Close adherence to a Mediterranean diet improves endothelial function in subjects with abdominal obesity. The American Journal of Clinical Nutrition, 90, 263-268.
  • Resnick, H. & Howard, B. (2002). Diabetes and cardiovascular disease. Annual Review of Medicine, 53, 245-267.
  • Rodrigo, R., Prat, H., Passalacqua, W., Araya, J., Guichard, C., & Bächler, J. P. (2007). Relationship between oxidative stress and essential hypertension. Hypertension Research, 30, 1159-1167.
  • Sales, M. M., Campbell, C. S., Morais, P. K., Ernesto, C., Soares-Caldeira, L. F., Russo, P., ... Simões, H. G. (2011). Noninvasive method to estimate anaerobic threshold in individuals with type 2 diabetes. Diabetology & Metabolic Syndrome, 3, 1-8.
  • Sales, M. M., Russo, P., Moreira, S. R., Santana, H. A. P., Moraes, J. F. V. N., Asano, R. Y., ... Campbell, C. S. G. (2012). Resistance exercise elicits acute blood pressure reduction in type 2 diabetics. Journal of Exercise Physiology online, 15, 98-109.
  • Santana, H. A., Moreira, S. R., Neto, W. B., Silva, C. B., Sales, M. M., Oliveira, V. N., ... Simões, H. G. (2011). The higher exercise intensity and the presence of allele I of ACE gene elicit a higher post-exercise blood pressure reduction and nitric oxide release in elderly women: an experimental study. BMC Cardiovascular Disorders, 11, 1-8.
  • Sharma, J. N. & Narayanan, P. (2011). Hypertension and diabetes: contribution of the kallikrein-kinin system. Journal of Diabetes & Metabolism, 8, 1-5.
  • Simões, H. G., Denadai, B. S., Baldissera, V., Campbell, C. S. G., & Hill, D. W. (2005). Relationships and significance of lactate minimum, critical velocity, heart rate, deflection and 3000m track-tests for running. The Journal of Sports Medicine and Physical Fitness, 45, 441-451.
  • Simões, H. G., Hiyane, W. C., Benford, R. E., Madrid, B., Prada, F. A., Moreira, S. R., ... Campbell, C. S. (2010). Lactate threshold prediction by blood glucose and rating of perceived exertion in people with type 2 diabetes. Perceptual and Motor Skills, 111, 365-378.
  • Simões, H. G., Moreira, S. R., Moffatt, R. J., & Campbell, C. S. G. (2010). Métodos para identificar o limiar anaeróbio em indivíduos com diabete tipo 2 e em indivíduos não-diabéticos. Arquivos Brasileiros de Cardiologia, 94, 71-78.
  • Stabler, T., Katherine, A. K., Ham, K., Jelesoff, N., & Allen, J. (2010). Potential mechanisms for reduced delivery of nitric oxide to peripheral tissues in diabetes mellitus. Annals of The New York Academy of Sciences, 1206, 101-106.
  • Teodoro, B. G., Natali, A. J., Fernandes, S. A. T., & Peluzio, M. C. G. (2010). The aerobic physical exercise intensity influence on the atherosclerotic. Revista Brasileira de Medicina do Esporte, 16, 382-387.
  • Tsikas, D. (2007). Analysis of nitrite and nitrate in biological fluids by assays based on the Griess reaction: appraisal of the Griess reaction in the L-arginine/nitric oxide area of research. Journal of chromatography. B, Analytical technologies in the biomedical and life sciences, 851, 51-70.
  • Wild, S., Roglic, G., Green, A., Sicree, R., & King, H. (2004). Global prevalence of diabetes: estimates for the year 2000 and projections for 2030. Diabetes Care, 27, 1047-1053.
  • Correspondence:
    Ricardo Yukio Asano and Herbert G Simões
    Programa de Pós-Graduação Stricto Sensu em Educação Física da Universidade Católica de Brasília
    EPTC, QS 07, LT 1, BL G, Sala 116
    Águas Claras, Brasília 72.022-900 DF, Brasil
    Phone: +55 (11) 97011-5500
    Email:
  • Publication Dates

    • Publication in this collection
      04 Oct 2013
    • Date of issue
      Sept 2013

    History

    • Received
      30 Mar 2013
    • Accepted
      17 May 2013
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    E-mail: motriz.rc@unesp.br