Safety of hyperbaric oxygen therapy in patients with heart 2 failure: A retrospective review

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Introduction
Hyperbaric oxygen therapy (HBOT) is an evidence-based intervention used to treat a variety of elective conditions, in addition to its role as an emergency treatment for carbon monoxide toxicity, decompression sickness, and arterial gas embolism (S1 Table) (1).The safety profile of HBOT is very favorable: although minor side effects related to increased environmental pressure and/or systemic hyperoxia can occur (e.g., claustrophobia, transient myopia, or middle ear barotrauma) (2)(3)(4), serious treatment complications (e.g., seizures, pulmonary oxygen toxicity, or pulmonary edema) are extremely rare (5).Anectodical evidence has suggested that patients with decreased left ventricular ejection fraction (LVEF) may be at an increased risk of acute heart failure (HF) during HBOT (6).Although this risk has not been substantiated by robust evidence, left ventricular (LV) systolic dysfunction has traditionally been considered a relative contraindication to HBOT (6).
Several hemodynamic changes are known to occur during and immediately after hyperbaric oxygen exposure (7).HBOT increases cardiovascular afterload, with associated increases in systolic and mean arterial blood pressure (BP), while cardiac output (CO) decreases due primarily to a decrease in heart rate (HR).Previous literature characterizing the effect of HBOT on CO is summarized in Table 1.
Table 1.Previous studies characterizing the effect of hyperbaric oxygen therapy on cardiac output.

Study
(% compared to baseline) Whalen, 1965 (8) -13 3.04 Pisarello, 1987  Numerous mechanisms for the effect of HBOT on CO have been suggested (13,14) although this effect predominately results from HBOT-induced vasoconstriction, the physiological protective response to extremely high arterial partial pressures of oxygen (7).These hemodynamic changes appear to be well tolerated in patients without preexisting cardiac disease (15,16).However, there is limited evidence regarding the applicability of HBOT in patients with HF and reduced ejection fraction (HFrEF) and, furthermore, no data on patients with HF with preserved ejection fraction (HFpEF) or HF with mid-range ejection fraction (HFmEF).We aimed to examine the safety of HBOT for patients with preexisting diagnoses of HF. .

Definitions
In accordance with the Canadian Cardiovascular society guidelines (17), HF was defined as a clinical syndrome in which abnormal heart function results in (or increases the risk of) clinical symptoms and signs of reduced cardiac output and/or pulmonary or systemic congestion either at rest or with stress.Chronic HF represents the persistent and progressive nature of the disease, whereas acute HF is defined as a change in HF signs and symptoms resulting in the need for urgent therapy.Recent guidelines proposed a new and revised classification of HF according to LVEF (18)(19)(20), which includes: (i) HF with preserved ejection fraction (HFpEF) = LVEF ≥ 50%; (ii) HF with mid-range ejection fraction (HFmEF) = LVEF 41-49%; and (iii) HF with reduced ejection fraction (HFrEF) = LVEF ≤ 40%.
. HFpEF is diagnosed in patients with signs and symptoms of HF as the result of high LV filling pressure, despite preserved LVEF (≥ 50%) (18).These patients also display normal LV volumes and an abnormal diastolic filling pattern (diastolic dysfunction) (18,21); therefore, HFpEF is sometimes referred to as diastolic heart failure (22,23).

Participants and data collection
We included all patients 18 years of age or older with a history of HF, regardless of EF, undergoing elective HBOT during the study period.To further categorize these patients, LVEF measurements via echocardiography were identified (where available) and used to stratify patients into three groups: (i) HFpEF = LVEF ≥ 50%; (ii) HFmEF = LVEF 41 -49%; and (iii) HFrEF = LVEF ≤ 40% (17).Each patient's demographic variables, past medical history, and medications were extracted from medical charts.Additional data extracted during the treatment period included HBOT indication, treatment pressure, total number of HBOT sessions, and adverse events associated with HBOT, including subjective symptoms reported by the patients and reported into the medical chart.All patients described in the study provided written consent to undergo HBOT for a clinical indication approved by Health Canada.

Hyperbaric oxygen therapy protocol
Conventional HBOT protocols were utilized in the treatment of all patients, as previously described (15): these included the administration of 100% oxygen at 2.0 or 2.4 atmospheres .absolute (ATA) for 90 minutes, with 1 -2 air breaks (0.21 fraction of inspired O 2 at the same ATA) per session, five times weekly, either in a mono-place chambers (Sechrist 3600H and Sechrist 4100H, Sechrist Industries Inc., Anaheim, CA, USA; PAH-S1-3200, Pan-America Hyperbarics Inc., Plano, TX, USA; Sigma 36, Perry Baromedical, Riviera Beach, Fl, USA) or through a plastic hood in the multi-place chamber (rectangular Hyperbaric System, Fink Engineering PTY-LTD, Warana, Australia).Standard monitoring included measurements of systolic (SAP), diastolic (DAP), and mean (MAP) blood pressure (BP), heart rate (HR), and peripheral oxygen saturation (SpO2) assessed during a five-minute period preceding and following each HBOT session.BP was measured non-invasively using an upper arm cuff and automated sphygmomanometer (Connex VSM 6000, WelchAllyn-Hill-Rom, New York, NY, USA) with the patient in a sitting or semi-sitting position.

Outcomes
The objective of this study was to evaluate the safety of HBOT among patients with known HF.The primary outcome was to describe any clinical signs or symptoms of acute heart failure occurring during and immediately after HBOT.Secondary outcomes included other treatment complications, assessed as the number of patients experiencing HBOT-related adverse or serious adverse events, such as barotrauma, oxygen toxicity (either central nervous system or pulmonary), ocular changes, or confinement anxiety.

Statistical analysis
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Qualitative data including patient demographics and past medical history characteristics were summarized using descriptive statistics.Continuous data were expressed as means ± standard deviations.

Acute cardiovascular complications
We observed symptoms consistent with HBOT-related HF in two patients (2/23, 9%).One patient with HFrEF (LVEF 24%) developed dyspnea after their fourth treatment for a diabetic foot ulcer.He had a history of hypertension, non-ischemic dilated cardiomyopathy, left ventricle hypertrophy, moderate pulmonary hypertension, mild tricuspid regurgitation, moderate diastolic disfunction, atrial fibrillation, peripheral vascular disease, obesity, diabetes, and kidney failure (not on dialysis).A routine random B-type Natriuretic peptide (BNP) collected one month before HBOT was 402 g/mL (Lab reference range: <= 99.9 pg/mL).Following HBOT, examination revealed an increased work of breathing and crackles consistent with pulmonary edema, without peripheral oxygen desaturation.In the emergency department, his BNP was measured at 1580 pg/ml, and he was managed with increased oral diuretics but did not require hospitalization.This patient later disclosed that he had voluntarily held his diuretics before the treatment to avoid .needing to urinate while inside the hyperbaric chamber.He subsequently continued HBOT, completing a total of 33 sessions without further complication.
A second patient, with HFpEF (LVEF 74%), developed dyspnea and desaturation after the sixth treatment session (also for a diabetic foot ulcer), ultimately requiring hospital admission.
He had a history of hypertension, type 2 diabetes on insulin, obesity, coronary artery disease with HFpEF, and mild diastolic dysfunction (on double diuretic therapy).His hypertension was reported as well controlled on dual therapy (nifedipine and telmisartan), but a review of his BP measured before and after each session revealed a consistently increased SAP (mean 155 ± 11 mmHg) and normal DAP (77 ± 4 mmHg) before each treatment, and both an increased SAP (170 ± 3 mmHg) and DAP (86 ± 10 mmHg) following each treatment.During the acute episode following his sixth HBOT session, acute coronary ischemia and pulmonary embolism were clinically excluded.A diagnosis of pulmonary edema in the context of HFpEF was made on the basis of an elevated BNP (143 pg/mL), pulmonary congestion identified through bedside lung ultrasound and chest X-ray, and normal LVEF with the presence of diastolic dysfunction on transthoracic echocardiogram.The patient's symptoms subsided after administration of an intravenous loop diuretic (furosemide), and he was discharged home in stable condition.
However, he elected not to resume HBOT.Three years later, he died of an unrelated oncologic pathology.
No acute cardiovascular complications were observed among the other 21 patients.

Other complications
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A total of seven non-serious adverse events were recorded: five instances of middle-ear barotrauma, and two of confinement anxiety.In each case, appropriate coaching and treatment were provided, and all patients continued HBOT without further complication.

Discussion
In this study we investigated whether patients with a history of HF can safely receive HBOT.Two patients in our cohort (9%) experienced acute symptoms of heart failure in relation to HBOT.One had a history of HFrEF, which portends a theoretical risk with respect to HBOT.The other had a history of HFpEF, which has not been previously reported to increase cardiac risks of HBOT.

Heart failure with reduced ejection fraction
HBOT is known to negatively impact cardiac output (CO), even among healthy patients (24).The decreased CO, along with an increased afterload resulting from systemic vascular resistance, has been hypothesized to be the cause of pulmonary edema reported in patients with reduced EF (6).In our cohort, among seven patients with HFrEF, only one developed signs of acute heart failure following HBOT.This patient had a severely impaired LVEF below 30% and he was receiving treatment with loop diuretics, although for two days he had been withholding his morning doses.With appropriate coaching and therapy optimization (an increase in the dose of .his loop diuretic), he continued HBOT and was able to complete 29 additional sessions without further complication.Our experience with these seven patients indicates that HBOT may exacerbate pulmonary congestion in patients with reduced ejection fraction, but also supports the feasibility of cautious treatment with close monitoring in this population after optimization of diuretic therapy.Interestingly, more recent studies have analyzed the long-term effects of HBOT on myocardial function, and paradoxically support a possible positive effect of HBOT on LVEF and other echocardiographic measures over longer time horizons (25)(26)(27).

Heart failure with preserved ejection fraction
One of the 13 patients with HFpEF in our cohort developed acute signs of heart failure after six HBOT sessions.He had a history of hypertension, previous admission for heart failure, echocardiographic evidence of diastolic dysfunction, and ongoing treatment with thiazide diuretics but not loop diuretics.His consistently increased SAP and DAP post-sessions may suggest a marked increase in afterload during and after each session (15), and increased afterload is a well-known effect of HBOT which contributes to decreases in CO (6,12).Further, there is evidence that hyperoxia increases LV end-diastolic pressure (LVEDP), and it is associated with disturbances of both early and late phases of LV filling in patients with and without HF (28).As a result, it is possible that a combination of increased afterload and impaired ventricular relaxation in the context of preexisting diastolic disfunction might represent the mechanism of the pulmonary congestion exacerbation in this patient. .

Complications of HFpEF resulting from HBOT have not been previously reported, although
this finding is important as HFpEF is more prevalent among older adults, women, and those with obesity, systemic arterial hypertension, diabetes mellitus, and renal dysfunction (29).Given the aging population and the increased medical complexity of patients seen in modern hyperbaric centres, the authors expect an increasing frequency of HBOT candidates with HFpEF in the hyperbaric medicine setting.

Clinical implications
Our data suggest that a minority of patients with HF, regardless of EF, may develop acute heart failure symptoms.However, we also show that this event is rare and potentially preventable, and that these patients can complete HBOT safely after therapy optimization, with close surveillance before and after each session.Cardiac guidelines recommend the use of loop diuretics in patients with HFpEF and HFrEF, aiming to reduce symptoms of congestion (18,20).In our study, no complications were observed among 21 patients out of 23.Interestingly, all but one of these patients were either on therapy with loop diuretics or receiving regular dialysis.It is possible that optimizing medical therapy (e.g., initiating or titrating loop diuretics) for patients with HFpEF may avoid or further limit pulmonary congestion in the setting of HBOT.
Some HF patients may present for HBOT without the typical history of HF symptoms and low LVEF, well known to physicians as pathognomonic of HFrEF.Indeed, HFpEF is diagnostically challenging for a clinician, given the frequency of atypical symptoms and/or an unremarkable LVEF.In our study, 54% of patients with HFpEF did not have a prior hospitalization primarily However, there is currently a paucity of evidence to define the feasibility or cost-effectiveness of routine cardiac screening before HBOT to prevent these complications.
Finally, both patients who experienced HBOT-related HF in our study developed symptoms after several treatment sessions, rather than after the first one, suggesting the possibility of a cumulative effect of HBOT on pulmonary congestion (rather than acute onset, severe pulmonary edema in a patient who is incidentally referred for HBOT on the brink of this complication).This observation warrants particular consideration in the care of HF patients undergoing HBOT: despite undergoing several uneventful treatment sessions, these patients may .gradually worsen, and still require close surveillance for the entire duration of treatment.Further research is needed to characterize the optimal management of patients with HF undergoing HBOT.

Limitations
Our retrospective study has several inherent limitations.Because we retrospectively reviewed health records already compiled at the time of HBOT, it is possible that not all pertinent risk factors were identified and recorded.Our data relate to a cohort of patients treated in two urban centres, potentially limiting their generalizability to other settings; similarly, patients were treated by several different healthcare professionals at these settings, limiting consistency in measurement and reporting.Importantly, our study design cannot appreciate patients with HF who may have been referred for HBOT, assessed, and considered to be at too great a risk to proceed with treatment.Additionally, due to the rarity of patients with HF undergoing HBOT, we report on a small sample size, limiting estimates of the incidence of HF exacerbation related to HBOT, and subgroup analyses (e.g., stratified by EF %) present data on even smaller groups of patients.Finally, the primary outcome of the study was observational, and while two patients experienced symptoms of acute HF following HBOT with a close temporal relationship this cannot prove a causative relationship, especially considering the presence of possible confounding variables (e.g., types of and adherence to diuretics, changes in treatment pressure, and positioning after the complication). .

Conclusion
Patients with a history of heart failure, whether HFpEF or HFrEF, may develop symptoms of pulmonary congestion during or after HBOT.However, they can safely complete HBOT following medical optimization with close attention paid to any clinical or pharmacological changes during treatment.Identifying patients at risk of HF exacerbation, and taking these measures to prevent acute symptoms during treatment, is an important objective of the pre-HBOT medical assessment. .
Abbreviations: CO = cardiac output, ATA = absolute atmospheres of pressure.
period, 23 patients with a documented diagnosis of HF received elective 151 HBOT.

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caused by their HF, and the diagnosis was based on transthoracic echocardiogram and signs and/or symptoms of HF while undergoing investigations for other indications (e.g., acute coronary syndrome, or additional tests required during dialysis or diabetes management).Therefore, even in the absence of a known impairment in LVEF, particular attention to any changes in the patient's clinical condition and pharmacological management during HBOT is warranted, and even mild-to-moderate respiratory or cardiac symptoms during HBOT should trigger further investigation to rule out an acute or subacute episode of HF.Patients with multiple comorbidities treated with numerous medications should be aware that any changes in their medications during HBOT should be discussed with their hyperbaric physician.For the same reason, the availability of a baseline echocardiogram to facilitate evaluation of diastolic dysfunction during the initial assessment, rather than relying on other tests traditionally performed prior to HBOT (e.g., electrocardiogram or chest x-ray), may further reduce the risk of patients with unrecognized HF developing symptoms in the context of HBOT.
This is a retrospective longitudinal cohort study of patients with HF who underwent elective HBOT between June 2018 and December 2020 in two Hyperbaric Medicine Centers in Ontario, Canada (Toronto General Hospital, Toronto; Rouge Valley Hyperbaric Medical Centre, Scarborough).Institutional Research Ethics Board approvals (CAPCR ID: 19-5081.1;IRB ID:2023-3194-14092-4) were obtained for study team members to collect data from medical records (last access to data on March 31, 2023; all authors but one (SS) did not have access to information that could identify individual participants during or after data collection).

Table 2 . Baseline demographics, comorbidities, and medications of the patient cohort. n= 23
Table 2 summarizes patients' details and HBOT characteristics.

Table 3 . Hyperbaric oxygen therapy details.
48%) were delivered at 2.4 ATA.Table3summarizes details of treatment for each a total of 906 HBOT sessions.Each patient underwent an average of 39 ± 17 treatments, and half . of them (434; 176