Critical Illness Clinical Trial
Official title:
Functional Electrical Stimulation-assisted Cycle Ergometry in Critically Ill: Linking Deranged Muscle Physiology to Long-term Functional Outcome
ICU acquired weakness contributes (ICUAW) to poor functional outcome in survivors of critical care. Most damage occurs during the first week of critical illness when patients are unable to cooperate with conventional active rehabilitation. Functional electrical stimulation-assisted cycle ergometry (FES-CE) may improve muscle function and long-term outcome. Methods: Assessor-blinded pragmatic single-centre randomized controlled trial. Adults (n=150) mechanically ventilated for < 48 hours from 4 ICUs who are estimated to need >7 days of critical care will be randomized to receive either FES-CE-based intensified rehabilitation or routine care, which will continue until ICU discharge. Primary outcome: Quality of life as measured by SF-36 score at 6 months. Secondary outcomes: functional performance at ICU discharge, cross sectional muscle diameter and nitrogen balance, and muscle power. In a subgroup we will assess insulin sensitivity and perform skeletal muscle biopsies to look at mitochondrial function, fibre typing and regulatory protein expression in response to FES-CE.
Background. Functional disability, a natural consequence of weakness, is a frequent and
long-lasting complication in survivors of critical illness. Over recent decades, mortality
from acute critical illness has decreased with a consequent increasing number of ICU
survivors. Understanding the post-ICU morbidity experienced by these survivors has become
increasingly important. The greatest burdens that survivors of critical illness face are
related to neuromuscular dysfunction and neuropsychological maladjustment. In particular,
neuromuscular abnormalities during critical illness are common, with a median prevalence of
57%. In both patients with chronic critical illness and survivors of severe critical illness,
neuromuscular weakness may be substantial and persistent, resulting in important decrements
in physical function and quality of life for years after discharge. In the past, routine
features of general care provided in the ICU included liberal use of sedation and
immobilization of the patient, which were thought to be necessary for facilitating
interventions to normalise physiological function by artificial means. Recently, there has
been a paradigm shift away from this approach towards a more conservative treatment
philosophy for patients in the ICU. This paradigm shift is consistent with the observation
that long-term physical problems in survivors of critical illness, particularly those with
respiratory failure, may result from the protracted ICU stay and period of immobilization
during which the patient is receiving organ support that is essential for survival. In line,
daily interruption of sedation policy has been widely adopted and proven to be beneficial and
early mobilization culture is spreading quickly across ICUs. Indeed, these strategies,
together with early physical therapy are the only safe and effective interventions in the
prevention of long-term neuromuscular disability in survivors of intensive care. It should be
stressed that in these studies, early rehabilitation is defined as starting between day 2-5
of ICU stay or as an activity beginning before ICU discharge. Standard early rehabilitation
cannot be started early enough, and functional electrical stimulation-assisted cycle
ergometry may be a solution to this dilemma.The first week on the ICU is critical as muscle
mass and function is lost quickly. Immobility-associated muscle loss is evident as early as
within18-48 hours of onset of acute critical illness or severe injury and is greatest during
the first 2 to 3 weeks of critical illness. Up to 40% loss of muscle strength can occur
within the first week of immobilization, with a daily rate of strength loss between 1.0% and
5.5% A 10-14% decrease in cross-sectional measurements of the rectus femoris muscle has been
observed within the first week of ICU stay. Conventional rehabilitation during the first few
days in the ICU is indeed limited in patients who are sedated and mechanically ventilated,
and typically consists of passive limb movements, with or without the use of stretch reflex
provided the earliest (within 48 hours of intubation) and largest dose of rehabilitation
(26±14 min a day for patients on mechanical ventilation) and reported improvements of
physical function at hospital discharge, but no measurements beyond. Active rehabilitation is
delayed until the neurological condition of the patient improves enough to facilitate
participation. In the sickest patients, who are at particular risk of developing ICUAW,
sedation and immobility may be prolonged well beyond first week, when established damage to
the muscle has already occurred. In order to achieve maximum efficacy, passive cycling and
neuromuscular electrical stimulation (NMES) can be delivered simultaneously and synchronised
to produce a coordinated pattern of movements. The technique is called FES-CE (functional
electrical stimulation-assisted cycle ergometry). There is a large body of experience with
these methods in the rehabilitation of patients with stroke and spinal cord injuries. The
method is effective in preventing the loss of muscle mass and has been shown to improve
anabolic resistance and insulin sensitivity in quadriplegic patients. In critical illness,
pilot studies have shown NMES itself (without synchronization and the use of bicycle) to be
safe, feasible and effective in maintaining muscle strength and mass. The only study of
FES-CE in critically illness is the pilot trial of Parry et al., where the feasibility and
safety of FES-CE was demonstrated in a small cohort of critically ill patients (8 patients
received the FES-CE intervention, versus 8 controls). Patients in the intervention group
showed significant improvements in the Physical Function in Intensive Care Test and a faster
recovery of functional milestones (e.g. time to stand from lying, and walking on the spot).
Hypotheses H1: As most of the damage to the structure and function of skeletal muscle occurs
during the first week, intensified rehabilitation, which includes FES-CE and starts within 48
hours after ICU admission, improves functional outcome of ICU survivors at 6 months when
compared to the routine standard of care. H2: Intensified early rehabilitation compared to
routine standard of care, shall preserve muscle mass and improve muscle power at ICU
discharge. H3:Intensified early rehabilitation compared to routine standard of care shall
increase insulin-mediated whole-body oxidative glucose disposal and mitochondrial functional
indices. Sample size calculation:In studies of critical illness outcome at 6-months using
36-Item Short Form Health Survey (SF-36) scores, the standard deviation varied between 10-13
points. In order to have 80% power to detect 5 point difference in SF-36 score between
control and intervention at the level of significance p<0.05 in the population with standard
deviation (SD) of 13, we would need 108 subjects (54 in each arm). In order to allow for
deaths and dropouts, the plan is to randomize 150 subjects.
Randomization. As soon as possible, but always within 48 hours of admission, participants
will be randomly assigned (1:1) to receive either standard care or the intervention using
offsite-independent randomization protocols (www.randomization.com). Randomization will be
stratified according to presence or absence of sepsis and the availability of a biopsy at
baseline. Concealed allocation will be performed using sequentially numbered opaque sealed
envelopes only accessible by research personnel with no involvement in the trial.
Once consent/assent is obtained, and prior to randomisation; participants will be referred to
a study physiotherapist who will administer baseline testing of muscle mass/cross-sectional
area (CSA) using diagnostic ultrasound (US), and baseline blood samples will be taken Both
groups will receive usual best medical and nursing care in the ICU, which include daily
sedation holds when applicable and delirium management as usual in the routine practice.
Respiratory physiotherapy will also be delivered without alterations. The routine standard
care arm will undergo mobilisation/rehabilitation delivered by personnel not involved in the
study in a usual, routine way. Details of physiotherapy treatment will be recorded but not
protocolled in the standard care arm. Intervention group In the intervention arm, early
rehabilitation is protocolled according to patients' condition and degree of cooperation and
there will be pre-defined safety criteria, which are in accordance with current
recommendations for active rehabilitation of critically ill ventilated adults. Whilst the
safety criteria are binding for the study physiotherapist, the rehabilitation protocol is not
and the delivery of physical exercise can be altered according to actual patient's condition.
However, any alteration and the reason for it will be recorded. The intervention will start
as soon as possible and always within 48 h of ICU admission, continuing until ICU discharge.
Supine cycling will be delivered as per protocol on supine cycloergometer attached to a
neuromuscular stimulator Surface electrodes will be applied to the gluteal, hamstrings,
quadriceps and calf muscles on both legs. The intensity of muscle stimulation will be
delivered at a level able to cause visible contractions (confirmed by palpation if uncertain)
in all muscle groups without causing undue pain or discomfort to the participant, according
to a regime specified by Parry, 2012. Once the patient is more alert, and able to
participate, they will be provided with standardized encouragement to engage in therapy. To
increase the intervention workload, resistance will be increased incrementally and cycling
cadence. If a participant is readmitted to intensive care, the intervention will be
re-initiated.
Study Procedures The ICUs are paperless and fully computerized, so vital functions and other
physiological parameters are monitored and data is routinely stored to secure hospital data
bases via a protected dedicated network. This includes data about nutritional intake and
urinary output. Urine samples will be collected daily, surfaced with toluene and stored in a
deep freeze facility for later determination of nitrogen content and 3-methyl histidine
levels (to calculate muscle catabolism rate and nitrogen balance). In addition, all study
patients will undergo an assessment by a study physiotherapist, which includes a measurement
of rectus muscle cross-sectional area on both legs and whenever the patient regains
consciousness, also muscle power by Medical Research Concil (MRC) score (standardized testing
of muscle power [0-5] on 12 muscle groups on all 4 limbs, giving the score 0-60 (60
suggesting normal muscle power). Blood will be taken, plasma separated and frozen at -80 C
for later analysis of cytokines and hormone levels. This assessment will be repeated at 7-day
intervals and at ICU discharge. At ICU discharge, the patients and relatives will be asked to
provide contact details for follow up. After 6 months, the patient or family will be
contacted for structured interview as required for SF-36 questionnaire, and collected using
Research and Development Organization (RAND) methodology. Whilst participants and
intervention physiotherapist cannot be blinded to group allocation, research staff assessing
outcome will be from separate clinical departments and thus remain blinded to treatment
allocation.
Complementary Studies: Insulin resistance and mitochondrial function These studies will be
performed in addition to other study procedures in a subgroup of patients, who give specific
consent to it. First measurement will be performed at baseline prior to randomization,
ideally the next morning after admission. Second measurement on day 7 of ICU stay, i.e. after
at least 5 days of intervention. Muscle biopsy. Will be performed from vastus lateralis
muscle by needle biopsy technique. The sample will be separated into three parts (50-100mg
each). One part will be immediately frozen in liquid nitrogen for analysis of protein/DNA
ratio and protein expression studies. The second part will be frozen in liquid
nitrogen-cooled isopentane for muscle fibre typing and immunohistochemistry analysis. The
third part put into culture media on ice for the preparation of homogenates and measurement
of citrate-synthase activity, spectrophotometric analysis of the activity of respiratory
complexes I-IV and western blot analysis of respiratory complexes. In the fresh muscle
homogenates, the investigators will use high-resolution respirometry to determine the
function of individual respiratory complexes in the cytosolic context and measure basic
functional metabolic indices. the investigators will specifically look at the degree of
mitochondrial uncoupling, respiratory chain capacity and the function of individual
complexes, including glycerol-3-phosphate shuttle. Frozen muscle samples will be stored at
deeply frozen for analysis of DNA/protein ratio, messenger ribonucleic acid (mRNA) and
proteins involved in the regulation of proteolysis, substrate oxidation and anabolic pathways
of skeletal muscle as well as immunohistochemistry and typing of muscle fibres. In addition,
the investigators will look at the change of these indices after seven days of critical
illness and the influence of the intervention vs. standard of care. the investigators will
look at correlation of these parameters with muscle power (i.e. compare bioenergetics profile
of skeletal muscle in those who develop ICUAW and in those who do not) and insulin
resistance. Insulin sensitivity and substrate oxidation will be measured after overnight
fasting by hyperinsulinaemic euglycemic clamp.
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