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METHOD AND APPARATUS FOR THE CONTROLLED DELIVERY OF GASES

20200188617 ยท 2020-06-18

    Inventors

    Cpc classification

    International classification

    Abstract

    A method of controlled delivery of breathing gases is described, during a first mode: the breathing gas inflow is predominantly through the first naris during inhalation; and the gas outflow is predominantly through the second naris during exhalation; and during a second mode that occurs after the first mode the breathing gas inflow is predominantly through the second naris during inhalation and the gas outflow is predominantly through the first naris during exhalation. The first mode and second modes are repeated. Also described is a system and apparatus implementing the method.

    Claims

    1. A method of controlled delivery of breathing gases, comprising: during a first mode: applying breathing gas pressure within a first naris of a mammal during inhalation; applying breathing gas pressure within a second naris of the mammal during inhalation, wherein the breathing gas pressure applied to the first naris during inhalation is higher than the breathing gas pressure applied to the second naris during inhalation and the breathing gas inflow to the mammal is predominantly through the first naris during inhalation; applying breathing gas pressure within the first naris of the mammal during exhalation; and applying breathing gas pressure within the second naris of the mammal during exhalation, wherein the breathing gas pressure applied to the first naris during exhalation is higher than the breathing gas pressure applied to the second naris during exhalation and the gas outflow from the mammal is predominantly through the second naris during exhalation; and during a second mode that occurs after the first mode: applying breathing gas pressure within the first naris of the mammal during inhalation; applying breathing gas pressure within the second naris of the mammal during inhalation, wherein the breathing gas pressure applied to the second naris during inhalation is higher than the breathing gas pressure applied to the first naris during inhalation and the breathing gas inflow to the mammal is predominantly through the second naris during inhalation; applying breathing gas pressure within the first naris of the mammal during exhalation; and applying breathing gas pressure within the second naris of the mammal during exhalation, wherein the breathing gas pressure applied to the second naris during exhalation is higher than the breathing gas pressure applied to the first naris during exhalation and the gas outflow from the mammal is predominantly through the first naris during exhalation.

    2. The method of controlled delivery of breathing gases as claimed in claim 1, wherein switching from the first mode to the second mode occurs after one breath cycle.

    3. The method for controlled delivery of gases as claimed in claim 1, wherein the breathing gas flow to and from the mammal is predominantly through a naris when the naris conducts between greater than 55% of the breathing gas flow.

    4. The method for controlled delivery of gases as claimed in claim 2, wherein the breathing gas flow to and from the mammal is predominantly through a naris when the naris conducts between greater than 55% of the breathing gas flow.

    5. A method of increasing inhaled nitric oxide in a mammal, comprising: during a first mode where a first naris of a mammal is a patent naris that passes a majority of airflow and a second naris of the mammal is a congested naris that passes less airflow than the patent naris: applying breathing gas pressure within the first naris of the mammal during inhalation; applying breathing gas pressure within the second naris of the mammal during inhalation; applying breathing gas pressure within the first naris of the mammal during exhalation; and applying breathing gas pressure within the second naris of the mammal during exhalation, wherein the breathing gas pressure applied to the first naris during inhalation is higher than the breathing gas pressure applied to the second naris during inhalation and the breathing gas inflow to the mammal is predominantly through the first naris during inhalation, and wherein the breathing gas pressure applied to the first naris during exhalation is lower than the breathing gas pressure applied to the second naris during exhalation and the gas outflow from the mammal is predominantly through the first naris during exhalation, and during a second mode pressures are switched to control the breathing gas inflow and outflow substantially through the second naris after a period of time greater than one breath cycle, and wherein during the second mode the second naris is the patent naris that passes a majority of airflow and the first naris is the congested naris that passes less airflow than the patent naris.

    6. The method for controlled delivery of gases as claimed in claim 5, wherein the breathing gas flow to and from the mammal is predominantly through a naris when the naris conducts greater than 55% of the breathing gas flow.

    7. The method of controlled delivery of breathing gases as claimed in claim 5, wherein the change in the pressures applied to the first and second naris is driven by a predetermined period that is user programmable, wherein the predetermined period is 1 minutes to 360 minutes, preferably the predetermined period is 1 minutes to 15 minutes, more preferably the predetermined period is 1 minutes to 5 minutes.

    8. The method of controlled delivery of gases as claimed in claim 5, wherein in the first mode the method forces the breathing gases inflow through the first naris and breathing gases outflow through the second naris.

    9. The method of controlled delivery of gases as claimed in claim 6, wherein in the second mode the method forces the breathing gases inflow through the second naris and breathing gases outflow through the first naris.

    10. The method of controlled delivery of gases as claimed in claim 8, wherein in the second mode the method forces the breathing gases inflow through the second naris and breathing gases outflow through the first naris.

    11. The method of controlled delivery of gases as claimed in claim 5, wherein the mammal is a human.

    12. An apparatus for the controlled delivery of breathing gases to a mammal, comprising: a fluid connection between a gases flow generator and each of a first and second naris of the patent; and a controller for controlling the pressure of the gases supplied to the first and second naris of the patent, the controller configured to automatically: during a first mode: applying breathing gas pressure within a first naris of a mammal during inhalation; applying breathing gas pressure within a second naris of the mammal during inhalation, wherein the breathing gas pressure applied to the first naris during inhalation is higher than the breathing gas pressure applied to the second naris during inhalation and the breathing gas inflow mammal is predominantly through the first naris during inhalation; applying breathing gas pressure within the first naris of the mammal during exhalation; and applying breathing gas pressure within the second naris of the mammal during exhalation, wherein the breathing gas pressure applied to the first naris during exhalation is higher than the breathing gas pressure applied to the second naris during exhalation and the gas outflow from the mammal is predominantly through the second naris during exhalation; and during a second mode that occurs after the first mode: applying breathing gas pressure within the first naris of the mammal during inhalation; applying breathing gas pressure within the second naris of the mammal during inhalation, wherein the breathing gas pressure applied to the second naris during inhalation is higher than the breathing gas pressure applied to the first naris during inhalation and the breathing gas inflow to the mammal is predominantly through the second naris during inhalation; applying breathing gas pressure within the first naris of the mammal during exhalation; and applying breathing gas pressure within the second naris of the mammal during exhalation, wherein the breathing gas pressure applied to the second naris during exhalation is higher than the breathing gas pressure applied to the first naris during exhalation and the gas outflow from the mammal is predominantly through the first naris during exhalation.

    13. The apparatus for the controlled delivery of breathing gases as claimed in claim 12, wherein switching from the first mode to the second mode occurs after one breath cycle.

    14. The apparatus for the controlled delivery of breathing gases as claimed in claim 12, wherein the breathing gas flow to and from the mammal is predominantly through a naris when the naris conducts between greater than 55% of the breathing gas flow.

    15. The apparatus for the controlled delivery of breathing gases as claimed in claim 13, breathing gas flow to and from the mammal is predominantly through a naris when the naris conducts between greater than 55% of the breathing gas flow.

    16. The apparatus for the controlled delivery of breathing gases as claimed in claim 12, wherein the mammal is a human.

    17. An apparatus for increasing inhaled nitric oxide in a mammal, comprising: a fluid connection between a gases flow generator and each of a first and second naris of the mammal; and a controller for controlling the pressure of the gases supplied to the first and second naris of the patent, the controller configured to automatically: during a first mode where the first naris is a patent naris that passes a majority of airflow and the second naris is a congested naris that passes less airflow than the forced patent naris: apply breathing gas pressure within the first naris of a mammal during inhalation; apply breathing gas pressure within the second naris of a mammal during inhalation; apply breathing gas pressure within the first naris of a mammal during exhalation; and apply breathing gas pressure within the second naris of a mammal during exhalation, wherein the breathing gas pressure applied to the first naris during inhalation is higher than the breathing gas pressure applied to the second naris during inhalation and the breathing gas inflow to the mammal is predominantly through the first naris during inhalation, and wherein the breathing gas pressure applied to the first naris during exhalation is lower than the breathing gas pressure applied to the second naris during exhalation and the gas outflow from the mammal is predominantly through the first naris during exhalation, and during a second mode pressures are switched to control the breathing gas inflow and outflow substantially through the second naris after a period of time greater than one breath cycle, and wherein during the second mode the second naris is the patent naris that passes a majority of airflow and the first naris is the congested naris that passes less airflow than the patent naris.

    18. The apparatus for increasing inhaled nitric oxide in a mammal as claimed in claim 17, wherein the breathing gas flow to and from the mammal is predominantly through a naris when the naris conducts greater than 55% of the breathing gas flow.

    19. The apparatus for increasing inhaled nitric oxide in a mammal as claimed in claim 17, wherein the change in the pressures applied to the first and second naris is driven by a predetermined period that is user programmable, wherein the predetermined period is 1 minutes to 360 minutes, preferably the predetermined period is 1 minutes to 15 minutes, more preferably the predetermined period is 1 minutes to 5 minutes.

    20. The apparatus for increasing inhaled nitric oxide in a mammal as claimed in claim 17, wherein in the first mode the method forces the breathing gases inflow through the first naris and breathing gases outflow through the second naris.

    21. The apparatus for increasing inhaled nitric oxide in a mammal as claimed in claim 17, wherein in the second mode the method forces the breathing gases inflow through the second naris and breathing gases outflow through the first naris.

    22. The apparatus for increasing inhaled nitric oxide in a mammal as claimed in claim 20, wherein in the second mode the method forces the breathing gases inflow through the second naris and breathing gases outflow through the first naris.

    23. The apparatus for increasing inhaled nitric oxide in a mammal as claimed in claim 17, wherein the mammal is a human.

    Description

    BRIEF DESCRIPTION OF THE DRAWINGS

    [0166] Embodiments of the present invention will now be described, by way of example only, with reference to the accompanying drawings, in which:

    [0167] FIG. 1 shows a graph of the normal bias in airflow between patent and congested nasal airways;

    [0168] FIG. 2 shows a graph of a nasal cycle spanning a 90 minute period;

    [0169] FIG. 3 shows a graph of a change in normal nasal airflow apportionment between the patent and congested airways when pressurised nasal breathing is introduced;

    [0170] FIG. 4 shows a graph of the variation of air pressure and resultant airflow passing through each naris during forced unilateral breathing of the present invention;

    [0171] FIG. 5 shows a graph of peak variation of inhalation air pressure differential between forced patent and forced congested airways measured at machine during forced unilateral breathing of the present invention;

    [0172] FIG. 6 shows a graph of the progression of titration pressure change from the commencement of operation;

    [0173] FIG. 7 shows a graph of the typical change in nasal resistance as a function of airflow rate;

    [0174] FIG. 8 shows a graph of the variation of air pressure delivered and resultant airflow passing through each naris during forced unilateral breathing of the present invention when pauses in breathing occur;

    [0175] FIG. 9 shows a graph of the change in nasal airflow apportionment ratio over each sleep stage;

    [0176] FIG. 10 shows a graph illustrating an example of differing time periods given to each phase of the nasal cycle;

    [0177] FIG. 11 shows a graph of variation of air pressure and resultant airflow passing through each naris during forced bilateral breathing in an embodiment of the present invention;

    [0178] FIG. 12 shows a graph the switch in airways carrying inhalation & exhalation phases of breath through each naris during forced bilateral breathing of the present invention;

    [0179] FIG. 13 shows a block schematic of one embodiment of the present invention;

    [0180] FIG. 14 shows a block schematic of a further embodiment of the present invention;

    [0181] FIG. 15 shows a diagram of a front view of a user wearing a mask with sensors on the mask strap;

    [0182] FIG. 16 shows a diagram of a front view of a user wearing a mask with alternative sensors on the mask strap;

    [0183] FIG. 17 shows a diagram of a side view of a user wearing a mask with sensors on the mask strap;

    [0184] FIG. 18 shows a full body diagram of a user showing the sensors of the present invention as they might be positioned on a user's body;

    [0185] FIG. 19 shows a graph of the gases inflow and outflow during a single breath;

    [0186] FIG. 20 shows a graph of the gases inflow and outflow during a breathing cycle;

    [0187] FIG. 21 shows a graph illustrating paranasal and iNO concentrations during normal nasal cycling;

    [0188] FIG. 22 shows a graph illustrating paranasal and iNO concentrations during absence of nasal cycling; and

    [0189] FIG. 23 shows a graph illustrating paranasal and iNO concentrations during sustained equal inter-nasal airflow apportionment.

    DETAILED DESCRIPTION

    [0190] Most healthy people experience, but are not aware of, a bias in nasal airflow where one nasal airway, termed patent conducts more airflow than the other which is described as congested.

    [0191] In this example illustrated in FIG. 1, the inhalation phase takes two seconds and exhalation spans a further four seconds.

    [0192] This bias in airflow passing through each naris varies in magnitude between individuals but normally the patent airway carries two thirds of the total tidal breath while the congested airway conducts the remaining one third. The status of each airway periodically swaps in what is commonly known as the nasal cycle, shown by FIG. 2. Here the previously patent airway becomes congested and vice-versa. This cycle normally has a period of approximately ninety minutes but can vary up to nine hours in duration.

    [0193] The ratio of tidal breathing air passing through each nasal airway can be manually controlled by either constricting or blocking airflow as it passes through each naris. For example, a finger is commonly used in Yoga techniques to manually restrict or completely occlude airflow through an individual naris. This method is commonly used to manually force change in the status of the nasal cycle.

    [0194] Nasal breathing of pressurised air also abolishes normal airflow partitioning. Here the patent airway experiences a reduction in airflow while the congested airway experiences an opposing response of increase in airflow, shown in FIG. 3.

    [0195] There are many issues associated with the abolishment of normal nasal airflow partitioning and the nasal cycle. From a functional perspective, the separate roles of air-conditioning and mucociliary clearance carried out by each airway are obliterated which results in both airways experiencing drying and ineffective mucociliary transport of entrapped pathogens. These phenomena are demonstrated by users of nasal applied continuous positive air pressure (n-PAP) therapy who commonly complain of symptoms associated with airway drying, inflammation and congestion.

    [0196] While supplementary humidification relieves these symptoms and helps to maintain mucociliary clearance in patients receiving n-PAP therapies, the influence nasal breathing of pressurised gases has on other physiological and neurological functions associated with nasal airflow partitioning and the nasal cycle are currently unknown. An indication of this influence can be found in some studies into n-PAP therapy adherence that has found, by choice, around 75% of patients use this therapy for less than 4 hours per night and around 50% discontinue long-term n-PAP use completely. Despite its popularity in relieving negative symptoms associated with airway drying, the ability of supplementary humidification to improve adherence to n-PAP treatment is questionable given no improvement occurs when supplementary humidification is introduced. These findings suggest that patient dissatisfaction with n-PAP therapy might be more complex than simply a case of mucosal drying. For example, abolishment of the nasal cycle might negatively influence sleep staging patterns or other physiological and neurological activity.

    [0197] The present invention system asserts control of nasal airflow during pressurised nasal breathing by regulating the apportionment of the total breath between each nasal airway during both inhalation and exhalation breathing phases. This control is achieved by varying the air pressure supplied to each naris in response to the continuous measurement of airflow passing to each naris and results in one airway, termed forced patent conducting a greater amount of airflow. The other airway conducts a lesser amount of airflow is termed forced congested.

    [0198] The pressure is preferably delivered through a substantially sealed mask that forms a seal with each naris or the face. The substantially sealed mask or system will also have a vent or bias flow to allow the exhaled air and CO2 to be flushed out, as used in conventional CPAP therapy systems that seal against the face, but also have a vent or bias flow.

    [0199] Alternatively the mask may be an open, unsealed, cannula type, similar to those used for oxygen delivery. When the system is set up for unsealed use it may take regular measurements of nasal airway resistance and follow the body's natural nasal cycle, as that is less likely to be abolished, due to the lower pressures being applied. Alternatively the system could cycle form left to right on a regular basis, as driven by the device program or user input. The user input maybe programmed, or may be an interface that the user pushes to change from one naris to the other due to the user experiencing discomfort. As the system delivers air predominantly to one naris at a time, it allows the other to recover, and rehydrate, while the other side is used to pass the air, oxygen, or other medication to the user's airway.

    [0200] Two generic types of nasal airflow control categories are envisaged along with two combinations: [0201] i. Forced unilateral breathing, where one airway conducts the majority of airflow during both inhalation and exhalation phases of breathing as demonstrated in the normal nasal cycle. [0202] ii. Forced bilateral breathing, where air exclusively passes into the nose though one naris during inhalation and then flows out of the nose through the other naris during exhalation. [0203] iii. Combinations of forced unilateral and bilateral breathing, where switching between these two types of breathing can occur in any order and arrangement. [0204] iv. Combination of forced unilateral breathing on inhalation and balanced nasal airflow on exhalation, where nasal airflow is partitioned during inhalation but forced to become equal during exhalation.

    [0205] When set to forced unilateral breathing mode, the present invention control system ensures that the forced patent airway receives a higher pressure than the forced congested airway during the inhalation phase of breathing. Conversely, during the exhalation phase, the patent airway receives a lower pressure than the forced congested airway. The present invention system also allows for the pre-setting of both the nasal cycle time duration and airflow partitioning between each naris. The delivery of maximal pressure also varies from when the system is first switched on to achieve measurement of natural nasal cycle status before entering into a pressure ramp phase that allows the user to acclimatise to breathing at augmented pressures.

    [0206] The present invention continuously regulates airflow through each naris so that the instantaneous amount of tidal breathing air passing through each naris achieves the desired percentage apportionment of the total airflow. As mentioned earlier, for a healthy awake person the airflow apportionment ratio for the patent airway is around two thirds of the total flow while the congested airway passes around one third, shown earlier in FIG. 1. This airflow apportionment ratio may vary from being near equal in both airways to exclusively passing through the patent airway.

    [0207] Artificially reinstating the natural nasal airway flow partitioning while on CPAP allows the nasal airway passages to function as they would do if the user was not on CPAP. For example it allows one side to humidify the air and the other to recover and conduct the mucociliary transport function. After a period of time the forced patent airway will change, as is normally does while not on CPAP. It may be possible to not use a water humidifier with the present invention CPAP system, as normal airway function can be resorted. Alternatively it may also be beneficial to include a water humidifier.

    [0208] Regardless of the airflow apportionment between the forced patent and forced congested airways, airflow bias in favour of the forced patent airway during pressurised nasal breathing is achieved by the present invention system providing different air pressures to each naris over the total breath cycle. During the inhalation phase of breathing the present invention system provides a higher pressure to the forced patent airway and a lower pressure to the forced congested airway. During the exhalation phase the forced congested airway receives a higher pressure than the forced patent airway. This relationship between individual naris airflow and air pressure supplied to each naris for one complete breath cycle is shown in FIG. 4.

    [0209] Change in the air pressure delivered to each naris can be progressive rather than a sudden switch, with change in pressure occurring in proportional to the amount of airflow occurring through each airway.

    [0210] While the therapy has many potential applications, the treatment method for obstructive sleep apnoea (OSA) is described below.

    [0211] While the different pressures delivered to each naris differ as a result of the individual's nasal airway response to pressure augmentation, the difference between these pressures also increases with increasing bias in airflow in favour of the forced patent airway. By way of an example, as shown by FIG. 5, during inhalation, the pressure difference between the patent and congested airways is around 0.4 cm H2O for the patent airway to conducts 55% of the total tidal airflow. The exhalation pressure trend may be different from that shown. This pressure difference needs to increase up to 2.1 cm H2O if the forced patent airway is to conduct 80% of the total tidal airflow. This data is for an individual at set pressure of 10 cm. The pressure differences at the machine become greater as the set, or titration pressure increases. It also decreases as the set pressure is reduced, for the same target ratio. These differences also vary from one individual to another, as they depend on nasal airway resistance.

    [0212] The maximal air pressure delivered to either naris varies from the time the system is first started is defined as treatment or titration pressure. There are three discrete pressure control stages over which the gas pressure being delivered is controlled: [0213] i. Measurement Phase. Here the system determines the current status of the patient's nasal cycle prior to treatment. This is done by initially applying an air pressure to both nares that supports normal breathing that could vary in pressure from very low (say 4 cm H2O) to titration pressure. During this time the individual naris airflow is simultaneously measured by the system over a set number of breaths (say 10). The phasing of the naturally occurring patent and congested nasal airways are then identified to either the left and right nares. [0214] ii. Ramp Phase. Immediately upon completion of the measurement phase the system responds in two ways. Firstly, the maximal pressure delivered to either naris ramps up over a pre-set ramp time (can vary from 0 to 60 minutes) until titration pressure is achieved. Secondly, the air is independently delivered to each naris over each phase of the breath cycle. During inhalation this airflow bias provides the patent airway with ramp pressure and the congested naris with a lower air pressure. Conversely during exhalation, the congested airway receives ramp pressure while the patent airway receives a lower pressure. During this phase of operation it may be desirable to switch the left airway to being forced patent if is not already in this status. It is also possible to gradually increase the ratio during the ramp phase, starting at 50:50 and going up to the desired ratio, or the ratio may be introduced at the end of the pressure ramp phase or both pressure and ratio ramp maybe independently controlled. [0215] iii. Treatment Phase. Once the ramp pressure equals the designated titration pressure the maximal pressure supplied to either naris over the full breath cycle is limited to the titration pressure. Here, both airways continue to be independently supplied differing air pressures in order to achieve the desired airflow partitioning ratio over each phase of the breath cycle as previously described in the ramp phase. Throughout the duration of the treatment phase there is also the ability to switch the status of each airway from being forced-patent to forced-congested. The relationship between each of these pressure phases is shown in FIG. 6.

    [0216] During the sleep period the designated titration pressure may vary. During the REM sleep phase the body loses muscle control while during n-REM sleep the brain regulates muscle action. Because of this, upper airway obstruction is most likely to occur during REM periods of muscle relaxation and less likely when muscle control is present.

    [0217] The next section describes the relationship between sleep stage and lateralisation of nasal breathing. Titration pressure may also vary depending on the nature of control algorithm implemented. This could vary from a steady value, as found in continuous positive air pressure (CPAP) applications, a reduction in titration pressure during exhalation as found in bi-level continuous positive air pressure (Bi-PAP) devices, through to adaptive pressure control based on detection algorithms as used in auto-setting continuous positive air pressure (A-PAP) therapy devices. Machine airflow measurements may be taken from one or both airflow streams leading to each naris and A-PAP detection may be based upon flattening of the waveform of measured airflow. A pressure relief function, where both airways experience a reduction in pressure but sustain a difference between each airway may also be included to reduce the exhalation effort.

    [0218] Phases i and ii previously described are optional and forced air flow partitioning may be implemented later in the treatment phase.

    [0219] The amount of air flowing through each nasal passageway is one factor in determining the individual airway resistance. Here, higher airflow rates cause an increased resistance while decreased flow leads to a reduction in resistance, as shown in FIG. 7. Because of this, the pressure difference delivered between the forced patent and forced congested airways can vary as the rate of air flowing through each naris varies.

    [0220] During periods of low airflow or where pauses in breathing occur the airflow resistance within each airway becomes extremely small. Under these conditions it becomes possible for air to be forced up one naris while air simultaneously exits out the other. This back-flow effect is driven by the difference in air pressure delivered to each naris. Because of this it is highly desirable during periods of low flow rates, or if complete pausing in breathing occurs, that there be no pressure differential delivered across both nares. The pressure change can be delivered in proportion to the measured airflow rate or by other means such as: [0221] Calculating the total inhaled air volume and using this measurement as a basis for determining when exhalation has completed and where airflow rates are low or have completely ceased. [0222] At a high level we will deliver the same pressure to each side whenever the patent flow (excluding the bias or vent flow) is below a threshold. For example when net flow in or out is less than 10 l/min for example. [0223] This threshold may vary and be a function of the pressure difference, and as the pressure difference is a function of the desired ratio, the threshold may vary as a function of the ratio. [0224] The pressure difference may step down to zero after reaching a threshold, or the pressure difference may be reduced gradually to zero. [0225] Another way to deal with this issue is to only introduce the pressure difference after a certain amount of time and after each inhalation has started, for example 0.3 seconds after the start of inhalation and only for a set amount of time, for example 1.0 seconds. This start will be determined by monitoring the flow signal. Or it could be maintained until the system estimates that the patients inhalation will end within a set amount of time, based on the flow signal (rate of change) and/or past breath cycles, for example within 0.3 sec of the end of the exhalation phase. The same could be repeated for the exhalation phase. [0226] Another variation may measure the rate of change of airflow rate near the end of the inhalation or exhalation breath phases. [0227] Another variation (that may apply to other embodiments in the application) is that only the inhalation flow ratio may be controlled and the exhalation phase may be conducted with the same pressure (or ratio) for left and right nares. This may allow for improved recovery of exhaled moisture while still only drying one side on inhalation. [0228] Still another variation is conducting the inhalation at the same pressure (or ratio) and controlling the exhalation phase to have different ratios.

    [0229] Any combination of these variations may be implemented. There are many instances where an individual may pause their breathing. This situation may occur during both awake and sleeping states and a breath cycle containing pauses is shown in FIG. 8.

    [0230] During periods where the user's breathing airflow is either very low or completely paused, as shown in FIG. 8, the system responds by delivering the higher level (titration) air pressure to both airways, thus preventing the potential for airflow to be driven through the airway receiving the higher pressure and out the airway receiving the lower pressure. If it were permitted to occur, this back-flow between airways would be very detrimental in maintaining airway hydration so it is essential that the system detects and reacts by delivering titration pressure to both airways during periods of low rates of breathing or during complete pauses in breathing.

    [0231] In all examples of ratio that are given, ratio could mean either an instantaneous flow ratio, or could be a ratio of tidal volume. For example flow rates may be measured instantaneously to control pressure instantaneously, or the area under the flow rate graph illustrated in FIG. 4 may be used to calculate the tidal volume for inhalation and exhalation (separately). This tidal volume from left to right could be compared to a target tidal volume ratio and pressure adjustments could be made to the next breath to reach the desired tidal volume ratio. Data from several breaths could also be used to control future tidal volumes, flow rates or pressures.

    [0232] The nasal cycle is set to discreet time periods (initially of 90 minutes duration but clinical studies may give rise to change) that align with the healthy pattern of neurological sleep stages given the correlation between the nasal cycle, cerebral dominance and sleep stage. The duration of time allocated to left and right nostril breathing dominance varies within each of these time periods as previously shown in FIG. 2. During entry into sleep the left naris airflow dominates and the shift to the left airway becoming patent during the initial treatment phase has been described earlier in the titration pressure ramp phase. Initially the amount of time allocated to each airway for each nasal cycle may vary over the sleep night. It seems that the amount of time for right naris dominant breathing increments over each progressive sleep period until there is an equal time allocated to left and right breathing. This initial best-guess setting is represented in FIG. 9.

    [0233] It is also envisaged that different cycle frequencies and durations could also be utilised during system start-up or to enable recovery from mouth leak or any other situation where the airways have suffered abnormal drying. It may be beneficial for rehydration to have a reduced period of nasal cycle, during periods of ramp or recovery from periods of mouth leak. For example the nasal cycle could be as short as one breath cycle 6 seconds or range up to more than 360 minutes

    [0234] The nasal cycle during ramp or any other phase may be user programmable, so the patient or clinician can select or pre-program the device, or preprogramed options may be selected based on the clinical or user need. Preferably the programmed nasal cycle is between 5 minutes and 360 minutes, even more preferably the programmed nasal cycle is between one and two natural nasal cycles. A natural nasal cycle typically being 90 minute, such that the programmed nasal cycle is between 90 minutes and 180 minutes. The cycle may vary during different phases, such as ramp or while at titration pressure. The total expected sleep time may be input, learnt from past nights data or based on an expected or set time of awakening in the morning, to compress or extend the ideal sleep staging in FIG. 9. The nasal cycle programming can be input to help achieve the desired physiological and neurological outcomes, such as sleep staging, or other body function that can be controlled or is linked to nasal airflow or nasal pressure variations. This may be useful in the treatment of the conditions listed below.

    [0235] It may also be beneficial to have periods where the ratio is controlled, to force airflow partitioning, and other periods were there is no partitioning. For example the device may use the airflow to sense if the patient is awake, as used in the Fisher & Paykel Healthcare Sense Awake technology, and deliver flow that is not partitioned while the patient is awake. Once the patient is asleep the airflow partitioning could be introduced. It may be that during periods of higher than expected flow, such as mouth leak or mask leak that the partitioning is turned off, until normal flow levels resume. Or it may be that air flow partitioning is introduced for periods to allow the nasal passages to recover before switching back to a non-partitioned state.

    [0236] As previously described, forced bilateral breathing is where air exclusively passes into the nose though one naris during inhalation and then flows out of the nose through the other naris during exhalation. In this case the nasal cycle has no relevance given each naris takes turns in passing the full tidal volume during the different breathing phases of inhalation and exhalation.

    [0237] When set to forced bilateral breathing mode the control system ensures that the airflow exclusively passes through one naris which is termed forced inhalation dominant. This is achieved by this airway receiving a higher pressure than the other during the inhalation phase of breathing. While actual pressures may vary, this same pressure relationship is maintained during the exhalation phase of breathing where the other naris that previously passed no air now exclusively passes the full amount of exhaled air. The nasal airflows and air pressures corresponding to this type of breathing is shown in FIG. 11.

    [0238] Just like the nasal cycle during forced unilateral breathing, the bilateral airflow designation for each naris for inhalation and exhalation phases of the breathing cycle may switch over a specified time period. This switch is shown in FIG. 12.

    [0239] There are many neurological and physiological pathological conditions where breathing therapy supplied using the present invention could provide a non-pharmaceutical alternative to current treatments or a new treatment option for previously untreatable ailments.

    [0240] While not limited to this list, a few of these conditions are listed below: [0241] i. Obstructive sleep apnoea. [0242] ii. Obesity. [0243] iii. Type 2 diabetes. [0244] iv. Stress/anxiety. [0245] v. Fatigue. [0246] vi. Sleep quality. [0247] vii. Cot death. [0248] viii. Maximising cognitive performance. [0249] ix. Infant and early childhood autism. [0250] x. Schizophrenia. [0251] xi. Stroke recovery. [0252] xii. Hypertension. [0253] xiii. Post-surgery recovery. [0254] xiv. Improved sport physical performance. [0255] xv. Improved long-distance travel recovery. [0256] xvi. Fibromyalgia. [0257] xvii. Alzheimer's disease. [0258] xviii. Migraine/tension headache.

    [0259] The system in the preferred embodiment would have a number of pre-programmable parameters, including the parameters listed below. [0260] 1. Measure Phase [0261] a. Measurement pressure. [0262] b. Measurement time. [0263] c. Swap to left airway time. [0264] 2. Pressure Ramp [0265] a. Left airway ramp time. [0266] b. Total ramp time. [0267] c. Titration pressure. [0268] 3. Treatment phase 1 [0269] a. Titration Pressure. [0270] b. Steady time. [0271] c. Swap time. [0272] 4. Treatment phase 2 [0273] a. Titration Pressure. [0274] b. Steady time. [0275] c. Swap time. [0276] 5. Treatment phase 3 (up to eight treatment phases)

    [0277] To enable a user or a physician to obtain information on the patient it is envisaged the system would have a number of readable parameters including: [0278] 1. Total and individual nasal airflow. [0279] 2. Time of use. [0280] 3. Individual pressures. [0281] 4. Airflow partitioning ratio.

    [0282] An embodiment of the invention will now be described with reference to FIG. 13. The device of the present invention 1 consists in a controller 2 having a processor, memory for storage including storing a control program and communication system for communicating with the connected sensors and other devices.

    [0283] The device 1 further has a gases flow generator 13 connected via pipe 13 and the air flow is split into pipe 12, 13 to a plurality of valves 9, 10. The valves 9, 10 are connected to the controller via communication lines 41, 42. Through each of the split pipes 11, 12 the gases eventually flow to a nasal mask having a connection 15, 16 to a naris. The gases flow to each naris of a user is separately controlled via the valve 9, 10 in the pipes which are fluidly connected to each naris.

    [0284] Additionally in the fluid connection to each naris there are airflow sensors 3, 4 and pressure sensor 5. The airflow sensors 3, 5 sense the airflow and communicate the airflow information to the controller via communication channels 43, 44. The pressure sensors 5, 6 sense the pressure and communicate the pressure the controller via communication channels 45, 46.

    [0285] Referring to FIG. 14 an alternative embodiment of the present invention will be described.

    [0286] The device 1 of the present invention in an alternative embodiment consists in a controller 2 having a processor, memory for storage including storing a control program and communication system for communicating with the connected sensors and other devices.

    [0287] The device 1 further has two gases flow generators 20, 21, each generator is in fluid communication with a single naris. The generators are also in communication with the controller via communication channels 47, 48. The channels allow the controller to both receive information from the gases flow generators 20, 21 and to control the gases flow generators 20, 21.

    [0288] The gases flow generators 20, 21 are connected via pipes 22, 7 and 23, 8 in fluid connection respectively to a single naris of a user. The gases flow to each naris of a user is separately controlled by the controller by the controller 2 controlling the gases flow generators 20, 21.

    [0289] Additionally in the fluid connection to each naris there are airflow sensors 3, 4 and pressure sensor 5. The airflow sensors 3, 5 sense the airflow and communicate the airflow information to the controller via communication channels 43, 44. The pressure sensors 5, 6 sense the pressure and communicate the pressure the controller via communication channels 45, 46.

    [0290] Also in communication with the controller 1 are various sensors. Referring to FIGS. 3 to 6 the system of the present invention optionally includes on the mask 31 that a user 34 wears EOG sensors 32, EEG sensors 47, ultrasound sensors 46 and an accelerometer 46. Referring to FIG. 18 body mounted sensors may optionally comprise ECG/EKG sensors 46, EMG sensors 45, respiratory effort bands 48, 49, EMG sensors 45 and a body mounted accelerometer 46.

    [0291] The various sensors described above are in communication with the controller 1 and allow the controller to make various assessments of the user using the system 1 of the present invention.

    [0292] The controller is able to detect nasal airway resistance measurement by for example setting the pressure for each flow generator 20, 21 shown in FIG. 14 to the same pressure, and measuring the flow in each side of the system, using airflow sensors 3, 4. Alternatively the pressure sensors 5, 6 and the airflow sensors 3, 4 could be used. As this measurement needs to interrupt the therapy for a period of time it may only be taken periodically for example every 1-10 minutes, and the test could last from 1 breath cycle to as long as 10 breathes cycles, or 6 second to 60 seconds. The relative resistance of each naris could be calculated by comparing the flow rates in each naris. Further the controller could measure nasal airway flow using the above described apparatus.

    [0293] Body position could be detected using the accelerometers 46 communicating with the controller 1 attached to the body and head of the user.

    [0294] Other physiological measurement could be taken such as Electroencephalography (EEG), Electrocardiography (ECG or EKG), electromyogram (EMG), respiratory effort bands, EOG, or any combination of these sensors.

    [0295] In one embodiment the present invention could be optimised to target maximize sleep efficiency. Sleep efficiency would be calculated by the controller using many of the previously described physiological measurements, with the controller 1 maximizing sleep efficiency by controlling the flow to each naris based on the measured data. In an alternative embodiment an individual patient's ideal nasal cycle frequency could be determined in and programmed into the controller.

    [0296] In another embodiment the present invention could be optimised to target a reduction in apnoea events. The controller 1 could monitor gases flow signal(s) to detect flow limitations or stops (apnoea event) in then adjust the gases flow and gases pressure via the valves 9, 10 or by controlling the gases flow generators 20,21. In another embodiment the controller could be programmed to switch the primary naris to reduce the rate of apnoea)

    [0297] In a further embodiment it may be predetermined that user has an ideal frequency of their individual nasal cycle, or that all people may benefit from the same nasal cycling, at a certain frequency, or that forced cycling is better than CPAP. This may allow each naris to rest and recover for a set period of time. This would allow the device to have a user, clinician or manufacturer programmed cycle. A nasal cycle shall be understood to mean the time taken for the primary naris to be patent and then congested, and back to be patented.

    [0298] The controller 1 of the present invention is programmed to over each breath cycle, regulate the inter-nasal airflow partitioning between each naris airway. In order to achieve this the controller 1 independently varies the air pressure experienced at each naris. Variation in this pressure is achieved through actuation of the two airflow regulation valves 9, 10 or controlling the gases flow generators 20, 21. The controller thus adjusts the amount of gases flowing through the air channels supplying each naris. Each airflow control valve 9, 10 or gases flow generators 20, 21 acts in response to controller 1 action. This control action is based on the sensed airflow measurement from within each air channel and is based on achieving the desired inter-nasal airflow partitioning.

    [0299] Differing air pressures are experienced at each naris to achieve a bias in inter-nasal airflow between each airway. This results in one airway experiencing airflow conditions that mimic it being actively being forced patent and the other forced congested throughout the whole breath cycle. This pressure offset experienced at each naris switches between airways during change in breath phases.

    [0300] During inhalation, the forced patent airway receives a greater air inflow from the air supply, causing its pressure to rise. On the other hand, the forced congested airway receives a lower air inflow from the gases supply and hence achieves a lower pressure than the other airway. This difference in mask pressure during inhalation causes a greater air in-flow to occur at the naris of the forced patent airway compared to that of the forced congested airway.

    [0301] During exhalation, the airflow into the nasal mask of the forced patent side is reduced by the controller, enabling the pressure to remains fairly stable and at near air supply pressure level. Conversely, the forced congested airway experiences an increase in gases inflow and hence achieves a higher pressure than that of the other airway. This elevation in pressure opposes air out-flow from the forced congested naris while the airflow from the forced patent naris experiences a lower opposing pressure force and hence less opposition to outflow. This swing in pressure between naris during exhalation maintains the desired airflow bias between each naris during this phase of the breath cycle.

    [0302] This inversion of pressure gradients experienced across the two airways during change in the phase of the breath cycle is essential to maintain the desired airflow bias between each of the nasal airways. The relationship between inter-nasal airflow partitioning and inter-nasal mask pressure over one breath cycle shown in FIG. 19.

    [0303] Periodically the controller 1 will switch the bias as discussed above to optimise the user's experience. Change in the bias in airflows occurring between each naris, termed switching, mimics the physiological change in the nasal cycle. This is achieved by progressively exchanging the control set points between airways over a designated time interval. The result of change in this parameter in terms of inter-nasal airflow partitioning is demonstrated by FIG. 20 in the region labelled switch phase.

    [0304] The system in one embodiment may regulate both inter-nasal airflow apportionment and time period of the nasal cycle and can also be used to elevate the levels of inhaled nitric oxide (inhaled nitric oxide) of a mammal in particular a human. This is realised by biasing the tidal airflow down one side of the nose, termed forced-patent, for a period of time to enable NO (nitric oxide) levels stored in the other side of the nose that experiences less tidal airflow, termed forced congested to increase. After a set period of time the sides of the nose receiving this bias in inter-nasal airflow apportionment is reversed, and in doing so mimics change in the nasal cycle. This set period can be between 1 and 360 minutes, preferably between 1 and 15, more preferably between 1 and 5. This forced change of inter-nasal airflow apportionment then forces the majority of tidal breathing air to pass through the previously forced congested side of the nose where stored NO levels are now high while the other side of the nose that was previously forced patent conducts a lesser amount of tidal breathing air which enables NO storage in the paranasal sinuses on this side to increase in concentration. This continual forced nasal cycling and bias in inter-nasal airflow apportionment elevates the user's inhaled nitric oxide level above that attained during normal nasal pressurised breathing such as that experienced during continuous positive airway pressure (CPAP) or ventilator assisted breathing.

    [0305] The status of the nasal cycle, where one nostril normally conducts more tidal airflow, termed patent, compared to the other, termed congested, allows the nose to simultaneously undertaking its air-conditioning and mucociliary roles. A healthy nasal cycle also enables the nose to act as a NO regenerator to maintain a higher mean concentration of iNO compared to a non-cycling nose. This is realised through the NO concentration within the paranasal sinuses on the congested side of the nose increasing as a result of low airflow whereas the NO concentration on the patent side paranasal sinuses are progressively depleted due to the higher airflow. Normal periodic change in the nasal cycle status results in the previously congested airway paranasal sinuses now having available a high concentration of stored NO so when this side of the nose becomes patent (where it conducts the majority of the tidal nasal airflow) there is a high concentration store of NO available to be inhaled. Conversely, the NO storage levels in the previously patent side of the nose, depleted due to the previously higher airflow, start to increase again due to the reduction in airflow when this side becomes congested.

    [0306] Referring to FIGS. 21 to 23, with time 21005 shown on all X axis and internasal airflow apportionment 21008, paranasal sinus NO concentration 21038 and maximum iNO 21068 shown on the all Y axis. The left and right nostrils are shown as 21010 and 21020. The left and right sinuses are shown as 21210 and 21220.

    [0307] FIG. 21 shows how this nasal cycle nostril NO regeneration effect enables a higher mean 21070 level of maximum iNO concentration to be entrained into the lungs compared to the case where there was no nasal cycle, shown by FIG. 22 (mean level 22070), and when near equal airflow passes down both nasal airways, such as that found during pressurised nasal breathing, shown by FIG. 23, (mean level 23070).

    [0308] In further embodiment the system can be configured for spontaneous breathing roles by operating in multiple modes including: [0309] 1. CPAP. [0310] 2. Bi-PAP. [0311] 3. Auto-PAP.

    [0312] The system may also be used for assisted breathing (ventilator) roles to deliver pre-defined therapeutic nasal tidal breathing patterns including those commonly found in yoga nasal breathing practice.

    [0313] Yoga nasal breathing practice involves inhaling through a first naris exhaling through a second naris, then inhaling through the second naris and exhaling through the first naris. The cycle is then repeated.

    [0314] Modes of operation could include but are not limited to: [0315] 1. Volume control. [0316] 2. Pressure control. [0317] 3. Proportional assist ventilation [0318] 4. Separate inhalation and exhalation timed tidal breathing with bias of inter-nasal airflow apportionment delivered to combinations of different or same nostrils.

    [0319] Augmented inhaled nitric oxide is intended to restore sympathovagal balance and also potentially bring a multitude of therapeutic benefits that include: [0320] 1. Post-operative recovery. [0321] 2. Pre-event build-for high-performance sports. [0322] 3. Aid post-event muscle recovery. [0323] 4. Aiding sleep homeostasis in the elderly or insomniacs. [0324] 5. Aid sleep onset for shift workers. [0325] 6. Assist ventilation and blood oxygenation in COPD sufferers. [0326] 7. Prevent the onset of metabolic disease and assist in the management of Type-2 diabetes. [0327] 8. Assist blood pressure reduction. [0328] 9. Long-term benefits in reducing cardiovascular disease. [0329] 10. Treat traumatic brain injury. [0330] 11. Treat neurological diseases such as Alzheimer's and Parkinson's.

    [0331] While the present invention has been illustrated by the description of the embodiments thereof, and while the embodiments have been described in detail, it is not the intention of the Applicant to restrict or in any way limit the scope of the appended claims to such detail. Further, the above embodiments may be implemented individually, or may be combined where compatible. Additional advantages and modifications, including combinations of the above embodiments, will readily appear to those skilled in the art. Therefore, the invention in its broader aspects is not limited to the specific details, representative apparatus and methods, and illustrative examples shown and described. Accordingly, departures may be made from such details without departure from the spirit or scope of the Applicant's general inventive concept.

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