ANZCTR - Registration

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Trial registered on ANZCTR

Registration number

ACTRN12623000240640

Ethics application status

Approved

Date submitted

15/02/2023

Date registered

6/03/2023

Date last updated

23/05/2023

Date data sharing statement initially provided

6/03/2023

Type of registration

Prospectively registered

Titles & IDs

Public title

Lidocaine Infusion Population Pharmacokinetics Study (LIPPS): determining pharmacokinetics of lidocaine in those undergoing breast reconstructive surgery

Scientific title

A trial to develop a population pharmacokinetics model for the administration of intravenous lidocaine to adult female patients undergoing breast reconstructive surgery

Secondary ID [1]

Nil Known

Universal Trial Number (UTN)

Nil Known

Trial acronym

LIPPS

Linked study record

Not Applicable

Health condition

Health condition(s) or problem(s) studied:

Pain Management

Condition category

Condition code

Anaesthesiology

Pain management

Anaesthesiology

Anaesthetics

Intervention/exposure

Study type

Interventional

Description of intervention(s) / exposure

Intraoperative intravenous bolus and infusion of lidocaine during breast reconstructive surgery.

Drug: Lidocaine 2%

Suitable candidates will be given an intravenous bolus dose of Lidocaine followed by an infusion for the duration of their surgery according to the following dosing parameters:

1) Intravenous bolus of (2.5mg/kg/LBW)/2 [2% lidocaine]
2) Intraoperative infusion of (3.33mg/kg/hr/LBW)/2 [2% lidocaine]
Lean body weight= (9270 x weight)/ (8780 + (244 x BMI))8
where BMI = total body weight/ (height in metres) = W / H2

W = total body weight in kg
H = height in metres.

Ideal body weight is capped at 68Kg.

The values entered into the Alaris PK pump program MUST be double checked against the printout from the drug dosing module by the research coordinator with the attending anaesthetist.

The bolus and infusion will be commenced at induction of anaesthesia and the infusion will be ceased at the completion of surgery. The exact duration of infusion is therefore dependent on operative considerations.

The dose of the intervention is determined by each individual patient's lean body weight.

The attending Anaesthetist will be responsible for the administration of the intravenous lidocaine. Patients will be under the constant supervision of an Anaesthetist throughout the duration of the infusion.
Samples to determine serum lidocaine concentrations will be taken at hourly intervals for the duration of the infusion, once in the Postoperative Anaesthetic Care Unit (PACU) and twice more between 8 and 26 hours post cessation of the infusion.

Intervention code [1]

Treatment: Drugs

Comparator / control treatment

No Control group

Control group

Uncontrolled

Outcomes

Primary outcome [1]

To establish the pharmacokinetics of lidocaine administered by intravenous infusion, as assessed by serial blood sample concentration determination. Parameters assessed will include the central and peripheral volume of distribution (VD), interdepartmental clearances, hourly clearance and elimination half-life (t½elim) of lidocaine when administered by intravenous infusion

Timepoint [1]

Serial serum lidocaine samples will be taken in study participants at specified time intervals to plot serum concentrations according to dosage and time. Samples will be taken hourly for the duration of the infusion, once postoperative in PACU and twice more (to examine elimination pharmacokinetics) between 8 and 26 hours post cessation of the infusion

Secondary outcome [1]

Incidence of treated bradycardia intraoperatively

Timepoint [1]

This outcome will be assessed continuously for the duration of surgery.
Information available from patient's recorded observations on the intraoperative monitor and Anaesthesia record. A record of treatment given will be taken from the patient's written Anaesthesia record. The patient's HR will be monitored by continuous ECG for the duration of surgery.

Secondary outcome [2]

Incidence of treated hypotension intraoperatively

Timepoint [2]

This outcome will be assessed continuously for the duration of surgery.
Hypotension will be recorded from the patient's monitor and/or the Anaesthesia record. Treatment given will be documented form the patient's Anaesthesia record. The patient will have a combination of non-invasive and invasive arterial blood pressure monitoring during the case

Secondary outcome [3]

Incidence of treated bradycardia in PACU

Timepoint [3]

This outcome will be assessed continuously for the duration of PACU admission.
Information will be obtained from the patient's recorded PACU observations where patients will have continuous ECG monitoring. Treatment given will be recorded from the patient's drug administration records

Secondary outcome [4]

Incidence of treated hypotension in PACU

Timepoint [4]

This outcome will be assessed continuously for the duration of PACU admission.
Information will be obtained from the patient's recorded PACU observations where patients will have intermittent non-invasive and/or continuous invasive blood press monitoring. Treatment given will be recorded from the patient's drug administration records

Secondary outcome [5]

Incidence of intraoperative infusion stopping events

Timepoint [5]

This outcome will be assessed continuously for the duration of surgery.
Information will be obtained from the intraoperative anaesthesia record. Where events has occurred, further information will be sought from the treating Anaesthetist where appropriate

Secondary outcome [6]

Incidence of suspected lidocaine toxicity events

Timepoint [6]

This outcome relates to the duration of the patient's hospital stay from the time of surgery to discharge. It will be assessed at the time of discharge.
Information will be obtained from the patient's medical records. Where an incident has occurred, the circumstances will be documented (presentation, treatment given, outcome etc). Further information may be sought from the treating team directly where appropriate

Secondary outcome [7]

Incidence of suspected SEVERE local anaesthetic toxicity events (generalised seizure, sudden unexplained loss of consciousness, life-threatening arrhythmia, cardiac arrest)

Timepoint [7]

Secondary outcome [8]

Incidence of Medical Emergency Team (MET) activation

Timepoint [8]

This outcome relates to the duration of the patient's hospital stay from the time of surgery to discharge. It will be assessed at the time of discharge.
Information will be obtained from the patient's medical records. Where the a MET review was required, the details will be recorded (reason for review and treatment given/outcomes if applicable). If required, further information may be sought from the treating team.

Secondary outcome [9]

Incidence of unplanned ICU, HDU or CCU admission

Timepoint [9]

This outcome relates to the duration of the patient's hospital stay from the time of surgery to discharge. It will be assessed at the time of discharge.
The reason form ICU admission, ( including relevant treatment and outcomes) will be recorded from the patient's medical records (both electronic and physical)

Secondary outcome [10]

Likely episodes of potential or actual lidocaine toxicity and safety endpoints set out above (and listed below for clarity) will also be assessed together as a composite secondary outcome.

1. Incidence of treated bradycardia intraoperatively, Information will be collected from the patient's recorded observations on the intraoperative monitor and/or the Anaesthesia record.

2. Incidence of treated hypotension intraoperatively, Information will be recorded from the patient's monitor and/or the Anaesthesia record.

3. Incidence of treated bradycardia in PACU, Information will be obtained from the patient's recorded PACU observations where patients will have continuous ECG monitoring.

4. Incidence of treated hypotension in PACU, Information will be obtained from the patient's recorded PACU observations where patients will have intermittent non-invasive and/or continuous invasive blood pressure monitoring.

5. Incidence of intraoperative infusion stopping events, Information will be obtained from the intraoperative anaesthesia record.

6. Incidence of suspected lidocaine toxicity events, Information will be obtained from the patient's medical records

7. Incidence of suspected SEVERE local anaesthetic toxicity events (generalised seizure, sudden unexplained loss of consciousness, life-threatening arrhythmia, cardiac arrest), Information will be obtained from the patient's medical records.

8. Incidence of Medical Emergency Team (MET) activation, Information will be obtained from the patient's medical records.

9. Incidence of unplanned ICU, HDU or CCU admission, Information will be obtained from the patient's medical records.

Timepoint [10]

Safety outcomes 1, 2 & 5 will be assessed continuously for the duration of surgery.
Safety outcomes 3 & 4 will be assessed for the duration of PACU admission.
Safety outcomes 6-9 will be assessed at the time of discharge

Composite data will be measured during data analysis, based on the data obtained individually, as listed above.

Eligibility

Key inclusion criteria

• Adult biological female patient aged >=18 and <80 years old
• Undergoing remote breast reconstructive surgery with a unilateral or bilateral DIEP (or other myocutaneous) flap
• ASA physical status 1-3

Minimum age

18 Years

Maximum age

79 Years

Sex

Females

Can healthy volunteers participate?

Key exclusion criteria

• Inability to provide informed consent – impaired cognition. Where consent cannot be obtained in English, an interpreter should be used to obtain informed consent
• Pregnancy
• History of epilepsy
• History of anaphylaxis, sensitivity or known contraindication to lidocaine or other amide local anaesthetics, including patients with porphyria and methaemaglobinaemia
• Baseline HR <50bpm or SBP <100mmHg
• Acute coronary event within the last 3 months
• Cardiac Conduction abnormalities including: Heart block (all degrees), Bundle Branch Block or Fascicular Block, Prolonged QT interval, Wolf Parkinson White Syndrome, channellopathy (e.g. Brugada Syndrome). A preoperative ECG is not mandatory.
• Abnormal serum sodium and/or potassium concentrations
• Active liver disease or abnormal liver function tests
• Medications within the last 7 days which affect lidocaine metabolism (amiodarone, beta blockers, cimetidine, fluoroquinolones, fluvoxamine, imidazoles, macrolides, verapamil, HIV drugs
• Cardiac Failure
• Severe renal disease (CrCl <30ml/min or dialysis dependent)
• Recruitment into LOLIPOP or any other Trial
• Planned regional anaesthesia/analgesia technique
• Co-administration of lidocaine within 24 hours of surgery (e.g. lidocaine patch)

Study design

Purpose of the study

Treatment

Allocation to intervention

Non-randomised trial

Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)

Not Applicable - this is an uncontrolled, non-randomised trial

Methods used to generate the sequence in which subjects will be randomised (sequence generation)

Not applicable

Masking / blinding

Open (masking not used)

Who is / are masked / blinded?

Intervention assignment

Single group

Other design features

Phase

Phase 4

Type of endpoint/s

Pharmacokinetics

Statistical methods / analysis

Data will be analysed using the first-order conditional estimation method with interaction. The pharmacokinetics of lidocaine will be described by a compartmental model parameterized in terms of clearance from the central compartment, apparent central and peripheral volumes of distribution (Vd) and intercompartmental clearances. It will include the assessment of parent-metabolite (MEGX, GX) models. Covariates such as patient demographics, body composition, plasma binding, phenotype and other covariates will be evaluated and included in the models. Model selection will be based on visual inspection of diagnostic scatter plots, the objective function value (OBJ) computed by NONMEM and biological plausibility of parameter estimates. All final models will be evaluated by performing a visual predictive check (VPC). Covariates will be evaluated for statistical significance using a stepwise forward addition and backward elimination process. The statistical criteria for retaining a covariate in the model will be p < 0.05 during forward addition and p < 0.01 for backward elimination. Five-hundred bootstrap runs will be conducted in order to assess the precision of final models’ parameter estimates. The final model will be evaluated by constructing prediction-corrected visual predictive checks (pcVPC), whereby the median, 5th and 95th percentile of the observed data will be compared against the median, 5th and 95th percentile of 1000 simulated versions of the original index dataset. Investigator Somogyi has published a similar type of modelling approach for ketamine and metabolites in treatment resistant depression.

Recruitment

Recruitment status

Not yet recruiting

Date of first participant enrolment

Anticipated

1/06/2023

Actual

Date of last participant enrolment

Anticipated

1/06/2024

Actual

Date of last data collection

Anticipated

1/07/2024

Actual

Sample size

Target

Accrual to date

Final

Recruitment in Australia

Recruitment state(s)

Recruitment hospital [1]

Royal Perth Hospital - Perth

Recruitment postcode(s) [1]

6000 - Perth

Funding & Sponsors

Funding source category [1]

Hospital

Name [1]

Royal Perth Hospital

Address [1]

Royal Perth Hospital
Victoria Square
Perth
WA 6000

Country [1]

Australia

Primary sponsor type

Hospital

Name

Royal Perth Hospital

Address

Royal Perth Hospital
Victoria Square
Perth
WA 6000

Country

Australia

Secondary sponsor category [1]

None

Name [1]

Address [1]

Country [1]

Ethics approval

Ethics application status

Approved

Ethics committee name [1]

Royal Perth Hospital Human Research Ethics Committee

Ethics committee address [1]

Royal Perth Hospital
Victoria Square
Perth
WA 6000

Ethics committee country [1]

Australia

Date submitted for ethics approval [1]

20/02/2023

Approval date [1]

20/04/2023

Ethics approval number [1]

RGS0000005943

Summary

Brief summary

We aim to develop a population pharmacokinetic model for lidocaine administration by intravenous infusion and identify clinically important covariates by conducting a prospective, single-centre, exploratory interventional study. It is anticipated that this project will provide data to inform a model which will facilitate accurate and potentially safer dosing of intravenous lidocaine. We plan to recruit 40 female adult patients undergoing breast reconstruction surgery. Patients will receive a bolus dose of lidocaine followed by an intravenous infusion. Dosing will be calculated using lean body weight and based on the dosing protocol approved and used in the LOLIPOP Pilot Trial (1) which has proven it to be safe and feasible. As an additional safety feature, we will be using half the dose of that used in LOLIPOP. This is because, unlike the LOLIPOP Trial, pain is not one of our outcome measures. Our primary aim of examining serial serum lidocaine concentrations and the potential formulation of a pharmacokinetic model is achievable at these lower doses. 
Lidocaine samples will be taken at hourly intervals throughout the duration of the infusion, and twice postoperatively between 8 and 26 hours of ceasing the infusion
 Current research (including the LOLIPOP Trial) is focussed on the analgesic properties of intravenous lidocaine. Several studies have already demonstrated a reduction in pain scores and a decrease in peri-operative opioid consumption. The goal of intravenous infusion is to establish and maintain therapeutic plasma concentrations of 0.5-5 mcg/mL, whilst avoiding higher doses that may result in toxicity.
Lidocaine has complex pharmacokinetics and demonstrates non-linear (time-dependent) pharmacokinetics with prolonged infusion, including increasing plasma concentrations and prolonging elimination half-life. Establishing a population-based pharmacokinetic model will facilitate a dosing regimen that maintains plasma lidocaine concentrations within a safe therapeutic window. This will improve the safety of intravenous lidocaine infusion by decreasing the risks of systemic toxicity, and potentially improve its efficacy by maintaining effective therapeutic plasma levels.

[1] Toner A.J. BMA, Schug S.A., Corcoran T.B. A pilot multicentre randomised controlled trial of lidocaine infusion in women undergoing breast cancer surgery. Anaesthesia. 2021.

ClinicalTrials.gov registration ID: NCT05072314

Trial website

Trial related presentations / publications

Public notes

This trial is not linked to a parent study. It is neither a sub-study or follow-up study.

However, lidocaine dosing is based on the Lidocaine dosing regimen approved and used in the LOLIPOP Pilot Trial and that is currently in use in the main multi-centre LOLIPOP Trial. Dosing will be 50% (half) of that used in the LOLIPOP Trials.

Contacts

Principal investigator

Name

Dr Peter Mc Cauley

Address

Research Department
Department of Anaesthesia and Pain Medicine
Level 4 Block R
Royal Perth Hospital
Victoria Square
Perth
WA 6000

Country

Australia

Phone

+61 0892241036

Fax

[email protected]

Contact person for public queries

Name

Peter Mc Cauley

Address

Research Department
Department of Anaesthesia and Pain Medicine
Level 4 Block R
Royal Perth Hospital
Victoria Square
Perth
WA 6000

Country

Australia

Phone

+61 0892241036

Fax

[email protected]

Contact person for scientific queries

Name

Tomas Corcoran

Address

Research Department
Department of Anaesthesia and Pain Medicine
Level 4 Block R
Royal Perth Hospital
Victoria Square
Perth
WA 6000

Country

Australia

Phone

+61 0892241036

Fax

[email protected]

Data sharing statement

Will individual participant data (IPD) for this trial be available (including data dictionaries)?

No/undecided IPD sharing reason/comment

Maintenance of patient confidentiality

What supporting documents are/will be available?

No Supporting Document Provided

Results publications and other study-related documents

Documents added manually

No documents have been uploaded by study researchers.

Documents added automatically

No additional documents have been identified.

Trial Review

Documents added manually

Documents added automatically