Pregnancy Clinical Trial
Official title:
Accuracy of Whole-Blood Testing for Rapid Detection of Pregnancy
It is common practice in the emergency medicine department to rapidly assess pregnancy status through the use of either urine or serum in pregnancy tests. Using whole blood instead of urine would facilitate a much more rapid emergency department identification of pregnancy status. No study to date has utilized whole blood for rapid detection of pregnancy status. Set in the busy adult emergency room at Maimonides Medical Center, this study will recruit a sample of women of reproductive age (18-55), who fit the inclusion criteria of being healthy and in need of a pregnancy test for own purpose or diagnostic testing/treatment. Blood samples will be taken from the participants and used in the hCG kits and the remaining blood was sent to the chemistry laboratory to perform the reference gold standard. The reference gold standard for a positive test is an hCG level >25mlU/ml. The research investigators and lab will be blinded to each other's results. Kappa statistics will be done for the measurement agreement between urine pregnancy results and whole blood pregnancy results, and whole blood results with laboratory results.
Background and Significance:
Point-of-Care testing to rapidly detect pregnancy in women of reproductive age is common
practice in Emergency Medicine departments. The patient history may not always reliably
identify the possibility of pregnancy1, and a large proportion of these patients are exposed
to potential teratogens because of their emergency department visit. In one study, 33% of
such patients received a radiographic evaluation and 75% were prescribed a medication2.
Additionally, a pregnancy test is required as the first step in the evaluation of a
suspected, potentially life threatening, ectopic pregnancy3.
Commercially available rapid immunochemical assays detect human chorionic gonadotropin (hCG)
concentrations >25 mlU/ml, and yield results at 3 minutes using urine and at 5 minutes using
serum4-6. However, in clinical practice these tests may take much longer to perform due to
significant delays in obtaining urine specimens from patients, or time delays required for
separating serum from whole blood. By prolonging patient waiting time for further diagnostic
testing and treatment, these delays may adversely impact on patient outcomes, emergency
department crowding, and patient satisfaction.
Using whole blood for hCG immunoassay, instead of urine or serum, would facilitate much more
rapid emergency department identification of pregnant patients. Whole blood can be obtained
immediately during intravenous insertion of phlebotomy, or by finger stick puncture using a
lancet in a manner similar to obtaining blood for bedside glucose determination.
Previous study of hCG immunoassays (which were less rapid than the immunoassays which are
now commercially available and in use today) utilized whole blood as well as urine and
serum, with equal sensitivities7. However, the accuracy of whole blood identifying pregnancy
using presently available rapid immunochemical hCG test kits has not been validated.
Objective:
To evaluate the sensitivity and specificity of a commercially available rapid immunochemical
hCG assay kit to detect pregnancy using whole blood specimens.
Material & Methods:
Design: A prospective, blinded study for validation of a diagnostic test
Setting: Two Clinical Sites:
1. Primary Care Women's Center of the Maimonides Medical Center, located at 5008 Fort
Hamilton Parkway, Brooklyn, New York.
2. Adult Emergency Department of Maimonides Medical Center, located at Fort Hamilton
Parkway and 49th Street, Brooklyn, New York.
Sample:
A convenience sample of healthy women from the above two settings, who meet the following
inclusion and exclusion criteria:
Inclusion Criteria:
1. Healthy adult women of child bearing age.
2. Who either request a pregnancy test, or require a pregnancy test for diagnostic studies
or treatment.
Exclusion Criteria:
1. Minors
2. Adults who are unable to independently give consent for study
3. Known pregnancy (i.e. - patient appears obviously pregnant)
4. Hemodynamically unstable.
5. Moderately to severely ill-appearing or in moderate to severe pain.
6. Technically not possible to obtain blood from the study subject.
Sample Size:
If we consider the quantitative hCG as the parameter for the final outcome: A sample of 279
from the positive group and 279 from the negative group achieve 80% power to detect a
difference of 0.0500 between the area under the ROC (receiver operating characteristic)
curve (AUC) under the null hypothesis of 0.8500 and an AUC under the alternative hypothesis
of 0.9000 using a two-sided z-test at a significance level of 0.0500. The data are discrete
(rating scale) responses. The AUC is computed between false positive rates of 0.000 and
1.000. The ration of the standard deviation of the responses in the negative group to the
standard deviation of the responses in the positive group is 1.000.
If we consider a dichotomous outcome for the qualitative result of hCG, instead of testing a
hypothesis: A sample size of 384 from each (Positive and Negative test) group will be
required to be 95% confident that the results would be within a true population parameter
using the following formula:
(Py)(Pn)
= N Std Error2 Py and Pn represent the proportion of people responding to each of the
categories in a dichotomous variable and N represent the sample size. We assumed a 50/50
split approach to maximize the variation (i.e. Py = 0.5 and Pn = 0.5) and a Type l error =
.05 to obtain a confidence interval of 95 percent.
Methods:
Prior to enrollment in this study, written informed consent will be obtained from all
subjects. After valid consent is granted, subjects will complete a brief standardized data
collection sheet to determine whether they meet eligibility criteria for participation in
this study. Study investigators will review this data. Subjects who meet eligibility
criteria and agree to participate in this study will be enrolled as participants. Each
participant will submit 5ml of whole blood to be used exclusively for this research study.
This blood specimen will be dram from an antecubital or other large upper extremity vein by
a physician, nurse, or professional phlebotomist. Each blood sample will be labeled with a
unique identification number. One or two drops from each blood sample will be used
immediately by the study investigator to perform an ICON 25 rapid hCG immunoassay test
(Beckman Coulter, Miami, Florida). The result will be read at 3 and 5 minutes and the
specimen identification number and corresponding result recorded in a log. The remainder of
each whole blood specimen will be sent to the Maimonides Medical Center chemistry laboratory
and processed to perform the reference gold standard test, a quantitative serum total hCG
(ADVIA Centaur® System total hCG chemiluminometric immunoassay; Bayer Corporation,
Tarrytown, New York) The Beckman Coulter ICON 25 kits is 100% sensitive and 100% specific at
hCG values > 25mlU/ml. Therefore, the reference gold standard for a positive pregnancy test
will be a quantitative serum hCG > 25 mlU/ml. Investigators who perform the whole blood
pregnancy test and laboratory technicians performing reference gold standard testing of
serum will be blinded to one another's results.
Confidentiality:
This study is not intended to evaluate the performance of any individual resident. Date from
this study will be used only for the statistical analysis for this study. The participant's
privacy will be maintained by giving each a unique ID number in the database for analysis.
Access to the database file will be protected by encryption and a password. All data forms
will be secured in a locked file cabinet and access will be limited to the investigators
only.
Data Analysis:
All data will be initially entered and analyzed via SPSS. Sensitivity and specificity will
also be estimated using 2X2 table.
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Observational Model: Case Control, Time Perspective: Prospective
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