Pulmonary hypertension is associated with a significant reduction in pulmonary artery pulsatility, contractility and elasticity, contributing to an increase in pulmonary artery pressure and pulmonary resistance. Using a hypoxic piglet model, this study demonstrated that improving pulmonary artery plasticity using a newly developed pulsatile catheter improves hypoxic pulmonary hypertension.
Pulmonary arterial hypertension (PAH) is a disease affecting distal pulmonary arteries (PA). These arteries are deformed, leading to right ventricular failure. Current treatments are limited. Physiologically, pulsatile blood flow is detrimental to the vasculature. In response to sustained pulsatile stress, vessels release nitric oxide (NO) to induce vasodilation for self-protection. Based on this observation, this study developed a protocol to assess whether an artificial pulmonary pulsatile blood flow could induce an NO-dependent decrease in pulmonary artery pressure. One group of piglets was exposed to chronic hypoxia for 3 weeks and compared to a control group of piglets. Once a week, the piglets underwent echocardiography to assess PAH severity. At the end of hypoxia exposure, the piglets were subjected to a pulsatile protocol using a pulsatile catheter. After being anesthetized and prepared for surgery, the jugular vein of the piglet was isolated and the catheter was introduced through the right atrium, the right ventricle and the pulmonary artery, under radioscopic control. Pulmonary artery pressure (PAP) was measured before (T0), immediately after (T1) and 30 min after (T2) the pulsatile protocol. It was demonstrated that this pulsatile protocol is a safe and efficient method of inducing a significant reduction in mean PAP via an NO-dependent mechanism. These data open up new avenues for the clinical management of PAH.
Pulmonary arterial hypertension is a life-threatening disease affecting the pulmonary vasculature. There is agreement in the field that an imbalance between an increase in vasoconstrictors (endothelin, serotonin) and a decrease in vasodilators (NO, prostacyclin) contributes to the development of PAH. Over time, this pro-constrictive phenotype evolves into a complex pro-proliferative and anti-apoptotic phenotype, contributing to the development of vascular lesions 1.
Prolonged exposure to vasoconstrictors leads to a significant and sustained increase in [Ca2+]i in pulmonary artery smooth muscle cells, allowing the activation of several calcium-regulated transcription factors, such as NFAT 2-4, promoting PASMC proliferation and resistance to an apoptosis phenotype 5. This phenotype leads to pulmonary vascular lesions, contributing to an increase in both PA pressure and pulmonary resistance, which ultimately leads to fatal right heart failure 6.
Currently, there is no treatment available that reverses PAH although there are several that improve patients’ quality of life 7. Among these treatments, the effectiveness of inhaled NO treatment has been demonstrated but because of its short half-life it is difficult to use in clinical practice. For this reason, more stable and durable treatments have been preferred, such as prostacyclin analogs, or endothelin receptor blockers 7. To develop better treatments, it is essential to improve and extend knowledge of the pathophysiology of PAH.
Pulsatility is a well-known stimulus activating shear stress-induced vasodilation, protecting the non-elastic distal artery from high-pressure flow injuries 8,9. In a model of PAH secondary to aortopulmonary surgical shunting, Nour et al. demonstrated intrapulmonary shear stress-mediated endothelial function enhancement 10. Several studies have demonstrated that NO, prostacyclin and ET-1 expression are closely regulated by changes in pulsatile flow. Indeed, a moderate increase in pulsatile flow increases eNOS activity and prostacyclin levels, both of which are reduced in PAH. Pulsatile flow modulation is probably implicated in the etiology of PAH and artificially increasing it is an attractive and novel way of increasing NO and prostacyclin production within the pulmonary circulation.
The present study aims to assess the effects of a 10 min pulsatile flow using a newly developed pulsatile catheter on hemodynamic measurements in a pulmonary hypertension (PH) model in piglets in whom hypoxia has been induced. It has been hypothesized that increasing pulmonary artery pulsatility induces vasorelaxation of the pulmonary arteries, thereby decreasing pulmonary artery pressure.
Right heart catheterization (RHC) is a critical clinical intervention for the diagnosis and follow-up of PAH patients. Indeed, it is the most reliable way of diagnosing PAH and allows physicians to assess vascular reactivity 11,12 as well as disease progression. In fact every PAH patient undergoes RHC several times. The present study in large animals aims to demonstrate the efficacy and safety of pulsatile catheters in assessing and treating PAH during a regular RHC procedure. Because pulsatile catheters are already available and RHC is routinely performed in PAH patients, this study provides all the information required to be able to conduct clinical trials rapidly.
NOTE: This study was authorized by Ethics committee number CEEA34.PB.103.12.
1. Use of Piglets as an Animal Model
2. Right Heart Catheterization
3. NO Measurement
4. Histology Measurements
Increasing Pulmonary Artery Pulsatile Flow Improves Induced Chronic Hypoxic Pulmonary Hypertension in Piglets
Prior to exposing animals to an increase in pulsatile flow, ultrasound was used non-invasively to check that the piglets had developed pulmonary hypertension. As shown in Figure 2, three weeks of chronic hypoxia induced the development of pulmonary hypertension in piglets, characterized by a significant reduction in pulmonary artery acceleration time (Doppler) and an increase in RV hypertrophy (M-mode). During RHC, invasive measurements of both right ventricular systolic pressure (RVSP) and mean PA pressure confirmed the presence of pulmonary hypertension in chronic hypoxic piglets vs. control piglets (values T0) (Figure 3). Diastolic pressure in the right ventricle was of -3 ± 1 mmHg in the control group and -2 ± 1 in the PAH group and the atrial pressure was -4 ± 2 mmHg in each group. The systemic pressure was 106 ± 13 vs 95 ± 18 mmHg in the control group vs the PAH group. Pulmonary hypertension was also confirmed by quantification of vascular remodeling on histological slices. To assess the probable therapeutic effect of pulsatile flow on pulmonary hypertension, a pulsatile catheter was used to generate an artificial pulsatile pulmonary flow for 10 min. As shown in Figure 3 an increase in the pulsatile flow for 10 min induced a significant reduction in both RVSP and mean PA pressure (T1 values) compared to baseline (T0 values). Since the cardiac output was not changed, pulsatility reduced the vascular pulmonary artery resistance by 26 ± 3% in the control group and by 41 ± 4% in the PAH group. To ensure that the decrease in PA pressure was sustained over time, animals in which the right catheter did not generate further pulsatile flow stayed in place for a further 30 min. As shown (T2 values), both RVSP and mean PA pressure continued to decrease compared to baseline (T0 values). It should be noted that systemic vascular parameters were not affected by the generation of pulsatile flow in the pulmonary artery and that neither systemic pressure nor cardiac output changed significantly.
Exhaled NO was measured for 6 chronically hypoxic piglets (T0) and 40 min after the generation of the artificial pulsatile flow (T2). This preliminary result, which needs to be confirmed – demonstrated a significant (p <0.001) increase in exhaled NO from 2 ± 1 ppm to 22 ± 8 ppm.
Finally, the pulsatile flow showed no significant effects on circulating ET-1 and 5-HT levels, suggesting that the decrease in PA pressure was mainly due to an increase in NO generation.
Figure 1: Diagram of the Protocol. (A) Diagram of the hypoxic box with the equipment required. (B) Timeline of the experiment. Echocardiographs were performed every week for 3 weeks before, during and after hypoxia. Please click here to view a larger version of this figure.
Figure 2: Echocardiography Results. Typical analysis measured non-invasively. (A) Over the 3 weeks (W1, W2, W3) of chronic hypoxia exposure (0.4 atmospheres), modifications in heart rate were observed as right ventricular hypertrophy progressively increased (B). In addition, pulmonary artery acceleration time (PAAT) measurements (C) demonstrated that PAAT decreased significantly in PAH piglets as PAH progressed, whereas no modifications occurred in the control group. An ANOVA statistical analysis adapted to the small number of animals concerned was performed (* p <0.05; ** p <0.005; *** p <0.001). Please click here to view a larger version of this figure.
Figure 3: Pulmonary Pressure was Reversed Following Pulsatile Catheter Exposure. (A) Piglets were exposed to pulsatile catheterization for 10 min. Mean pulmonary artery pressure (PAPcm H2O) was evaluated before (T0), immediately after (T1), and 30 min after the pulsation (T2). Each time, the pressure was measured over 10 stable cardiac cycles in order to obtain a representative value for the results. (B) Vascular remodeling was quantified and was increased in PAH piglets compared to control piglets. An ANOVA statistical analysis adapted to the small number of animals concerned was performed (* p <0.05; ** p <0.005; *** p <0.001).
Figure 4: Pulsatile Catheters did not Modify Hemodynamic Parameters. The systemic systolic pressure (A) and the cardiac output (B) were evaluated in PAH and control piglets before, during and after the pulsatile protocol. No significant difference was observed between the groups and the different times. (C) Systolic pulmonary pressures were measured (mmHg) by right catheterization at T0, T1 and T2. An ANOVA statistical analysis adapted to the small number of animals concerned was performed (* p <0.05; ** p <0.005; *** p <0.001). Please click here to view a larger version of this figure.
For the first time, it has been shown that changes in pulmonary pulsatile flow are causally related to the development of PAH secondary to chronic hypoxic exposure. This translational approach provides evidence that inducing an artificial increase in pulmonary pulsatile flow using a specifically designed catheter improves pulmonary hypertension, probably by increasing NO generation.
These findings are not only original, they are also of great therapeutic interest, demonstrating that endogenous NO production can be stimulated mechanically and safely within the pulmonary circulation without affecting systemic functions. The study design complies with the latest preclinical research recommendations in pulmonary hypertension, which have recently recommended tests on large animals before new methods are adopted in clinics. The translational potential of these findings is very high.
However the pathophysiological mechanism of PAH is not unique. Classification of PAH differentiates between five different groups. Group three is representative of medial hypertrophy secondary to chronic hypoxia. Although it can be included in this group, the model does not perfectly represent human PAH. Human PAH secondary to chronic hypoxia is mainly linked to chronic bronchitis in which lesions of the bronchi and pulmonary parenchyma induce peripheral pulmonary-to-systemic shunts. These shunts induce hypoxemia via a mechanism different to that used in the model. Here, the model is closer to life at high altitude than lung disease. However the cardiac hemodynamics of the model are close to those in humans: same heart rate, same cardiac output and same pulmonary pressure.
A previous study by Nour et al. demonstrated coronary 17 and pulmonary circulation 10 vasodilation secondary to pulsation. Their model of PAH was an aortopulmonary shunt. Aortopulmonary shunts increase blood flow in the pulmonary artery. It is our view that placing a balloon in the pulmonary artery creates an obstacle to right ventricular ejection that could interfere with the decrease in pulmonary pressure observed in their experiment. It is for that reason that a model of PAH was chosen that does not affect cardiac output. Instead the cardiac blood flow remains constant throughout the experiment.
Moreover, their experimental conditions are quite different since the chest of the animal is opened surgically during application of pulsatility, which modifies normal ventilation and pulmonary circulation. It is therefore difficult to compare the two experiments.
The mechanism via which pulsatility decreases PAH has not been demonstrated. The study conducted by Nour showed an increase in e-NOS, while we demonstrated an increase in exhaled NO. These two conclusions are strongly suggestive of a role played by NO in the PAH reduction mechanism. However other mediators may be involved 18. It would be useful to perform further studies to examine the biomarkers involved in pulsation-induced vasodilation.
NO delivery has been reported as being beneficial to PAH patients 19-21. However, NO has a very short half-life and its use to treat patients therefore involves a complicated procedure. In addition, the release of NO secondary to pulsatile flow needs to be more clearly demonstrated. The increase in eNOS and the systemic vasodilation observed in the study conducted by Nour but not in the study suggest that it is necessary to conduct further studies examining NO release induced by pulsatility and its role in vasodilation. This is another reason why NO therapy is not yet used in clinical practice.
Right heart catheterization is a standard procedure used to assess the severity of the condition and to monitor patient treatment 16,18. It would be entirely feasible to use pulsatile catheters instead of regular catheters. This would not require any additional procedures and could be used to assess the severity of PAH as well as to treat patients and improve their condition. Another advantage of this technique is that it has few, if any, toxic effects. Since these devices induce NO generation via a physiological process, any detrimental interaction with other therapies is unlikely. Consequently, pulsatile catheters could be rapidly and safely used in patients requiring ongoing treatment.
Although novel, the findings of this study confirm previous observations made in left heart failure patients who developed secondary pulmonary hypertension. Indeed, patients with pulmonary hypertension associated with chronic congestive heart failure have a significant risk of morbidity and death following heart transplants. Torre-Amione et al. 22 observed that patients who received a pulsatile left ventricular assist device had a significant decrease in pulmonary pressure, enabling them to qualify for heart transplants. Although not explored in the study, NO release could probably explain the improvement in pulmonary pressure, as in this study. This study not only confirms previous findings but suggests that the use of pulsatile catheters should also be explored in left heart failure patients who develop secondary pulmonary hypertension of high clinical significance.
Despite being very promising, this study has several limitations. Firstly, the efficacy of this device has only been tested with one model of pulmonary hypertension. Currently there are very few large animal pulmonary hypertension models 23. It is essential to develop new models. In the light of the findings by Torre-Amione et al. 22 concerning secondary pulmonary hypertension, a pulmonary hypertension model associated with left heart failure would be of great therapeutic interest. The effect of pulsatile catheters on NO release was estimated by measuring exhaled NO and not directly via the NO circulating in the PA. Ozkan et al. 24 have shown that exhaled NO is a good indicator of the amount of NO within the PA circulation. Indeed in their study, they demonstrated that exhaled NO decreased in PAH patients vs. controls and that stimulating NO generation in the PA using epoprostenol was reflected in the exhaled NO. This means that exhaled NO measurement is a valid method of estimating NO levels circulating in the PA. This study also measured PA pressure over 30 min, but the long-term effects (weeks, months and years) have not been studied. Sharing this technique will allow other teams to test different protocols (i.e. combinations with other treatments), analyze the benefits and perhaps discover adverse effects. Above all, it is hoped that this study may lead to rapid and safe use of the device in human PAH patients.
The authors have nothing to disclose.
The authors have nothing to disclose.
Drugs for anesthesia | |||
sodium thiopental, THIOPENTAL SODIUM | Abbott, France | 0000071-73-8 | powder 3 place Gustave Eiffe 94518 RUNGIS CEDEX. |
isoflurane, FORANE | Abbott, France | 05260-05 | glass bottle 250 ml 3 place Gustave Eiffe 94518 RUNGIS CEDEX. |
midazolam, Hypnovel | Accord Healthcare | Vidal | injectable ampoules 1mg/ml 45 Rue du Faubourg de Roubaix 59000 Lille France |
pramocaine,TRONOTHANE 1 % | Laboratoires LISAPHARM | Vidal | Gel appl locale T/30g 3, rue Scheffer. 75016 Paris. |
morphine chlohydrate Lavoisier | CMD Lavoisier Laboratoires CHAIX et DU MARAIS | Vidal | injectable ampoules 7, rue Labie -75017 Paris – France |
Acrylates Copolymer-Carbopol® Aqua SF-1 Polymer | Lubrizol | gel appl local Elysées La Défense 19 le Parvis 92073 Paris la défense |
|
Material | |||
Ventilateur Harvard 683 | Harvard apparatus | Harvard apparatus | DRIM 75 rue des Anglais – 78700 Conflans Ste Honorine |
Echographe Voluson E8 with a 3,5 MHz probe | General Electric | GEHealthcare | DRIM 75 rue des Anglais – 78700 Conflans Ste Honorine |
Pulsatil Catheter | Cardio inovating system | Cardio innovative systems, 33 rue Vivienne, Paris, France 75002 | |
NO breath Analyseur | Respur | Respur | 26 rue Felix Rouget 95490 Vaureal France |