Critical Illness Clinical Trial
Official title:
Insulin Resistance Versus Absolute Insulin Deficiency: Evaluating the Mechanism of Hyperglycemia in Pediatric Critical Illness
BACKGROUND AND PURPOSE
Critical illness hyperglycemia (CIH) - elevated blood glucose in the critically ill patient
population - has gained much interest among health care providers over the past several
years. Clinical studies in adults have documented a high rate of hyperglycemia in some
post-surgical and medical intensive care units (ICUs). However, the primary reasons for
interest in this topic are not due just to its high rate, but also to the fact that by
returning the high glucose levels found in this population to normal with insulin therapy
can dramatically improve clinical outcomes by decreasing both morbidity and long-term
mortality. Because of this, aggressive glucose control has become common practice in adult
ICU critical care management.
Although there is substantial data describing the high incidence of CIH in adult patients,
there is little information regarding this condition in children. A single retrospective
study recently published also suggested a high incidence of CIH in children with critical
illness secondary to both medical and surgical causes. It is yet to be determined if, like
in adults, normalizing blood glucose levels with insulin improves outcomes in this pediatric
population. Because evidence appears compelling that hyperglycemia is both common and
detrimental in adults, many pediatric ICUs have likewise begun to focus on aggressively
treating hyperglycemia in critically ill children.
The proposed study is a prospective observational pilot study to occur in the Pediatric
Intensive Care Unit (PICU) at Children's Healthcare of Atlanta at Egleston. This prospective
pilot study is being done to evaluate the endocrine factors associated with, if not
responsible for, CIH, and the changes that take place with the restoration of normal blood
glucose levels by insulin therapy.
To address these profound issues this study will pursue two interrelated Aims:
Aim #1: To determine if critical illness hyperglycemia is associated with absolute insulin
deficiency, peripheral insulin resistance, or both.
Aim #2: To characterize the requirement of insulin required to initially restore and
maintain normal blood glucose levels, and compare the changes in insulin that take place
with this normalization in patients with CIH.
We hypothesize that the hyperglycemic response to critical illness will be associated with
abnormally low levels of insulin as compared to patients without critical illness
hyperglycemia.
SUMMARY OF PROCEDURES
This will be an approximately 12 month long, single center, prospective study of patients
between ages 2 and 12 years old who meet criteria for CIH in our pediatric intensive care
unit during the period of enrollment. Patients will be screened by physicians and staff and
evaluated via inclusion and exclusion criteria, the evaluation will discussed with the
family/legal guardian by appointed critical care fellow, attending or physician appointee,
and the patient will be enrolled if informed consent is granted. Following informed consent
approval from family/legal guardian, blood samples will be collected and sent for storage
and processing in the clinical laboratory at Children's.
Three patient population groups will be assessed in this study:
- Group A - Study Patients - At risk for CIH/with CIH Labs will be drawn in our target
population at diagnosis of CIH and sent for insulin and C-peptide levels. These levels
will be repeated 24 hours after initiation of insulin, and then followed every three
days until insulin is no longer needed, then repeated once more 24 hours after insulin
is off (see protocol).
- Group B - Control Patients - At risk for CIH/without CIH Insulin and C-peptide levels
will be drawn in a control group of patients with the same risk factors but without CIH
at the time of admission, 24 hours after admission, then in 3 days.
- Group C - Control Patients - Not at risk for CIH/without CIH The same protocol of lab
schedules will be used in a second control group consisting of patients that are not
deemed at risk for critical illness hyperglycemia.
III. POTENTIAL RISKS
Most patients who meet criteria usually have an arterial line, central venous catheter, or
"blood drawing" IV. It will be rare that a separate venous puncture will be needed to
collect samples. If the blood to be collected, approximately 2cc per stick, is believed to
negatively impact the patient by either the patient or clinical caretakers, blood will not
be drawn.
Information collected in this study will contain Protected Health Information (PHI) on
subjects. There is the potential risk of unintentional disclosure of this information.
However, certain steps will be followed in this study minimalize PHI disclosure to help
protect the subjects' privacy and confidentiality. Once collected, this information will be
kept in a database that is password protected and with limited access on a
password-protected network. Other than institutions required by law to have access to
research records, only authorized research staff will have access to the research database
associated with the study. Furthermore, no data will be identifiable to study subjects, as
each subject will be assigned a unique study number when entered into a database. If
published or presented, no identifying features will be provided.
IV. POTENTIAL BENEFITS
There may be no direct potential benefit to the subjects participate in this study. However,
the information learned from this study may benefit other patients in the future.
V. INCLUSION AND EXCLUSION CRITERIA
Inclusion:
- All patients between ages 2 and 12 years of age admitted to the pediatric ICU who meet
criteria for critical illness hyperglycemia (ie: all patients on mechanical ventilation, all
patients on vasoactive medications, patients deemed otherwise "at risk" for CIH by attending
service) and are started on our standard CIH screening and treatment protocol will comprise
the pool of potential study candidates.
Exclusion:
- Certain patients who meet criteria for critical illness hyperglycemia and thus are started
on insulin will be excluded from this study: Age Patients less than 2 or greater than 12
years of age will be excluded from this study to decrease age variability.
Pre-existing known endocrine disorder Patients with known or suspected Type 1 diabetes will
be excluded because of their pre-existing absolute lack of insulin production secondary to
autoimmune β cell destruction.
Oncology patients Oncology patients will be excluded because of the effects of
immunosuppressants on study markers.
Renal replacement therapy Patients on continuous veno-venous hemofiltration (CVVH) or any
type of dialysis (intermittent dialysis, peritoneal dialysis) will be excluded as it is
unclear how different forms of renal replacement therapy affect insulin levels, and certain
types of dialysis affect glucose and insulin levels (i.e. dextrose containing PD fluid).
Non-adherence Inability or unwillingness of the legal guardian to provide consent, or
unwillingness of the child to provide assent.
VI. INFORMED CONSENT PROCESS
Patients will be considered eligible for this study at the discretion of the pediatric
intensivists or their appointees (i.e. pediatric critical care fellows or nurse
practitioners). There will be discussion with the family of the background information,
reasons for conducting the study, and the risks involved. At any time during the study there
will be opportunity to be removed from the study without impact on care. After all questions
have been answered, written informed consent will be obtained from the parents (or legal
guardian), and signed by the intensivist or appointee.
If the parent/subject decides not to participate, the child will continue with their
standard of care procedures as originally planned without any further testing.
As part of the ongoing informed consent process, whenever appropriate, the subjects
participating in this study will be provided with additional pertinent information after
initial time of consent.
;
Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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