Overview

Neurostimulation of Spinal Nerves That Affect the Heart

Status:
Unknown status
Trial end date:
2018-11-01
Target enrollment:
0
Participant gender:
All
Summary
The purpose of this study is to study the use of neurostimulation in chronic advanced refractory heart failure. The study is determine if it is safe to use neurostimulation in patients with chronic advanced refractory heart failure and to also determine initial observations with regards to its potential effect on heart function and quality of life. The investigators hypothesis is that this study will show both safe and positive effect of neurostimulation on heart failure patients.
Phase:
N/A
Accepts Healthy Volunteers?
No
Details
Lead Sponsor:
Jerry Estep, MD
Collaborators:
The Methodist Hospital Research Institute
The Methodist Hospital System
Criteria
Inclusion

1. Male or female ≥18 years;

2. Chronic heart failure NYHA class III-IV of ischemic and non-ischemic etiology;

3. Screening Left ventricular Ejection Fraction (LVEF) ≤ 30% measured at baseline by
echocardiography;

4. Screening 6 minute walk test score of less than 450 meters measured at baseline;

5. Hospitalization for heart failure or outpatient IV administration of inotropic agents,
human B-natriuretic peptide or IV diuretics within the past 12 months (stable for at
least 2 weeks);

6. On standard optimal medical therapy for CHF before medical therapy.*

7. No changes in active cardiac medications during the 1 week prior to treatment;

8. Written informed consent.

- Patients with current or prior symptoms of heart failure and reduced LVEF should
be on stable optimally uptitrated medical therapy recommended according to
current guidelines (Circulation. 2005; 112 (12): e154) as standard of care for
heart failure therapy in the United States. This minimally includes an
ACE-inhibitor (ACE-I) at stable doses for 1 month prior to enrollment, if
tolerated, and a beta blocker (carvedilol, metoprolol succinate, or bisoprolol)
for 3 months prior to enrollment, if tolerated, with a stable up-titrated dose
for 1 month prior to enrollment. This also includes an Angiotensin II Receptor
Blocker (ARB) at stable doses for 1 month prior to enrollment, if tolerated, when
ACE-I is not tolerated. Stable is defined as no more than a 100% increase or a
50% decrease in dose. If the patient is intolerant to ACE-I, ARB, or beta
blockers, documented evidence must be available. In those intolerant to both
ACE-I and ARB, combination therapy with hydralazine and oral nitrate should be
considered. Therapeutic equivalence for ACE-I substitutions is allowed within the
enrollment stability timelines. Aldosterone inhibitor therapy should be added
when NYHA Class III or IV symptoms occur on standard therapy. If aldosterone
inhibitor therapy is administered in Class II patients, it must be initiated and
optimized prior to enrollment. Eplerenone requires dosage stability for 1 month
prior to enrollment. Diuretics may be used as necessary to keep the patient
euvolemic.

Exclusion

1. Inability to comply with the conditions of the protocol;

2. Inability to perform cardiopulmonary exercise test due to mechanical physical
limitations

3. Presence of a transplanted tissue or organ or LVAD (or the expectation of the same
within the next 12 months);

4. Planned AICD or CRT within the next 12 months unless AICD is prescribed for primary
prevention

5. Pacemaker dependent patients.

6. Acute MI, CABG, PTCA, within the past 3 months

7. Chronic refractory angina or peripheral vascular pain;

8. Valvular heart disease requiring repair or replacement;

9. Need for chronic intermittent inotropic therapy;

10. Malignancy: evidence of disease within the previous 5 years;

11. Known HIV infection or immunodeficiency state;

12. Chronic active viral infection (such as hepatitis B or C);

13. Severe systemic infection: defined as patients undergoing treatment with antibiotics;

14. Active myocarditis or early postpartum cardiomyopathy (within the first 6-months of
delivery);

15. Systemic corticosteroids, cytostatics and immunosuppressive drug therapy
(cyclophosphamide, methotrexate, cyclosporine, azathioprine, etc.), DNA depleting or
cytotoxic drugs taken within 4 weeks prior to study treatment;

16. Patient is pregnant, of childbearing potential and not using adequate contraceptive
methods, or nursing.;

17. Patient scheduled for hospice care;

18. Any other medical, social or geographical factor, which would make it unlikely that
the patient will comply with study procedures (eg. Alcohol abuse, lack of permanent
residence, severe depression, disorientation, distant location and a history of
non-compliance).