Predictors of Opioid-Induced Respiratory Depression (OIRD)

Study Description

Brief Summary

Purpose of the Study: (1) To classify an individual subject's ventilatory response in terms of respiratory depression to a bolus of remifentanil under normoxic and hyperoxic conditions. (2) Measurement of specific respiratory parameters to predict the opioid-induced respiratory depression (OIRD) response.

Detailed Description

This study is using FDA approved drugs (remifentanil, oxygen and carbon dioxide) in an investigational manner and the study is also developing a diagnostic test that is currently investigational. Investigational means that the FDA has not approved the use of the drugs in this manner or the diagnostic test being developed.

Opioid-Induced Respiratory Depression (OIRD) is recognized as potentially life threatening and the cause of substantial morbidity (poor health) and mortality (death). Respiratory depression is when the amount of breathing you do in a minute falls below normal. Opioids are medications widely used to treat both acute (lasting hours to days) and chronic (lasting months) pain, both within and outside the hospital setting. Opioids have been used outside the prescribed circumstances resulting in misuse and abuse. Even within the controlled environment of acute hospital care it is difficult to identify those individuals at most risk of OIRD, as many do not possess physical characteristics, such as obesity or obstructive sleep apnea (stop breathing during sleep), which may predispose to OIRD. In the absence of the ability to easily identify at-risk individuals the Anesthesia Patient Safety Foundation have suggested that all patients receiving opioids must be considered at risk of OIRD and therefore require appropriate monitoring.

Even when fully awake, the normal response to breathing a gas mixture containing carbon dioxide (CO2) is to increase the amount of breathing. The effect is similar to breathing in and out of a paper bag. This is called the Hypercapnic Ventilatory Response (HCVR) and can be measured. Not everyone responds in an identical manner - there will be differences in the HCVR from one person to the next. But if an individual's baseline HCVR is measured, then the change from baseline can also be measured.

This study is being done to: (1) classify or rate an individual subject's ventilatory (breathing) response in terms of respiratory depression to a bolus of a potent opioid (similar to morphine, often referred to as a narcotic). The opioid used for this study is Remifentanil and is commonly used in the operating room. Remifentanil will be given under normoxic (breathing room air [21% Oxygen]) and hyperoxic (breathing 50% oxygen) conditions to (2) determine if the measurement of the specific respiratory parameters will predict the OIRD response.

Study Design

Outcome Measures

Primary Outcome Measures

1. Hypercapnic Ventilatory Response (HCVR) gradient based upon ETCO2 and Minute Volume [Sequence #1 approximately 30 minutes]

   Is there a correlation between the HCVR and susceptibility of OIRD.

Secondary Outcome Measures

1. The proportion of subjects who are classified as low, medium, or high risk for Opioid Induced Respiratory Depression (OIRD). [Sequence #2 approximately 1 hour]

   This will be measure in Low, Medium, or High.

Eligibility Criteria

Criteria

Inclusion Criteria:

• is between 18 and 50 years of age;

• weighs greater than 40 kilograms;

• is American Society Anesthesiologist (ASA) status 1 [assessment by PI or delegate];

• has a BMI between 18.0 and 30.0 [calculated from measured height & weight];

• has completed the appropriate fasting periods for solids and liquids prior to the administration of remifentanil

• and has provided written informed consent and is willing to comply with the study procedures.

Exclusion Criteria:

• has a prior or known allergy to lidocaine or similar pharmacologic agents;

• is currently taking any medication other than for birth control;

• is currently participating in, or has recently participated in (discontinued within 30 days prior to this study) in an investigational drug study [self-reported];

• has a negative Allen's Test to confirm patency of the collateral artery [clinical assessment by PI or delegate];

• has made a whole blood donation or has had at least 450 ml of blood drawn within 8 weeks prior to the study procedure [self-reported];

• is female with a positive pregnancy test [serum or urine], or is female and is unwilling to use effective birth control between the time of screening and study procedure;

• has anemia [measured by venous blood gas sample];

• has a history of sickle cell disease [self-reported];

• has a positive urine cotinine or urine drug screen or oral ethanol test [POC testing];

• has a history of narcotic or recreational drug addition [self reported by subject in response to questioning by PI or delegate; review of duke electronic medical history record];

• has room air saturation less than 95% by pulse oximetry [measurement by PI or delegate];

• has a clinically significant abnormal EKG [assessment by PI or delegate];

• has a clinically significant abnormal pulmonary function test via spirometry [assessment by PI or delegate];

• has a COHb greater than 3%, or MetHb greater than 2% [measured by venous blood sample co-oximetry];

• is intolerant to a breathing mask apparatus [assessment by PI or delegate];

• has any condition in the opinion of the investigator which would make him or her unsuitable for study participation [assessment by PI or delegate];

• is unwilling or unable to provide informed consent or comply with the study procedures;

• has Rayanud's disease.

Contacts and Locations

Locations

Sponsors and Collaborators

• Duke University

Investigators

• Principal Investigator: David MacLeod, MB BS, Duke Anesthesiology

Study Documents (Full-Text)

More Information

Publications