Patent Document

RELATED APPLICATIONS 
       [0001]    This application is a continuation of U.S. patent application Ser. No. 10/096,102, filed Mar. 13, 2002. 
     
    
     FIELD OF THE INVENTION 
       [0002]    The present invention relates to a system and method for evaluating testing methods. In particular, the present invention relates to a system and method for comparing two or more testing methods, systems, or products. The invention is particularly useful in the medical testing field, to determine if the methods, and any results obtained therefrom, are clinically equivalent. However, the invention could easily be applied to any laboratory situation in which measurements made under different conditions are compared in order to determine whether the different conditions alter the results in a significant way. 
       BACKGROUND OF THE INVENTION 
       [0003]    Clinical laboratories perform tests for doctors and healthcare professionals. The laboratories perform tests on human blood, urine, plasma, serum or other body fluids in order to measure chemical or physical properties of the specimens. The results of these tests are used by doctors and healthcare professionals to make clinical decisions related to patient care and treatment. Because results are used to make clinical decisions for patient care, dependable test results are of the utmost importance. 
         [0004]    Clinical laboratories purchase supplies and products in order to perform these tests. For example, blood collection tubes, needles, diagnostic instruments, chemical reagents and other supplies are used during testing, and therefore must be periodically replenished. From time to time, some element of a testing procedure may change for a variety of reasons. For example, a new blood collection tube type may replace an older version, new blood collection tubes may include a new additive, or a new blood collection tube could be made of plastic rather than glass. Chemical reagents may be ordered from a different supplier, or even a new batch of reagents could be considered a change in the testing procedure. Furthermore, the diagnostic instruments used to perform the testing themselves may change. Newer models may replace older testing equipment. Also, hardware, software and firmware updates may be applied to the equipment. 
         [0005]    Of course, the above-described list of variables in testing procedures is merely exemplary, and the list of possible variables is endless. It is important to recognize, however, that any change in testing procedure can potentially affect test results. Therefore, because the accuracy of test results is so important, there is a need for a way to gather and analyze empirical data to show that the testing procedure using the new method, device or system does not significantly affect the testing results. 
         [0006]    There is certain degree of variability in any testing procedure. By analyzing test data, it is possible to measure the variability in test results. In addition, a new test procedure or method may give results that are on the average different from a “reference” test procedure. This average difference is called bias. If the bias between a new test procedure and a reference method is small enough, and the variability in the results using the new procedure is no greater than the variability of the old test procedure, the new test procedure can be considered clinically equivalent to the old test procedure. There is presently specialty software on the market for evaluating and validating testing methods. However, the existing software products fall short in several respects. 
         [0007]    Currently, most if not all clinical laboratories rely on a statistical technique called linear regression to compare testing methods, systems or products. The linear regression analysis is almost always accompanied by a graphical representation called a scatter diagram. In a scatter diagram, the results from one method, system or product are plotted against the results from the “reference” method or system on a chart and linear regression analysis is used to determine a best-fit line on the chart to represent the data points. A perfect result on a scatter diagram would be a line having a slope of one and a vertical axis intercept of zero. Unfortunately, the degree to which the best-fit line fits the observed data depends on the number and frequency distribution of data values used. Therefore, the quality of the best-fit line for its accuracy and usefulness may be manipulated by selecting individuals at either end of some analytic spectrum and including their results in the data. Thus, while scatter diagrams and linear regressions may be helpful in determining the similarity of results between a reference and evaluation method, system or product, they are not sufficient. 
         [0008]    A commonly used quantity calculated by existing software packages is called R.sup.2, sometimes referred to as the coefficient of determination. R.sup.2 can have a value between 0 and 1, and represents the degree to which a straight line fits the data, relative to the total variability observed. A value of 1 indicates that all the points fit exactly on the same line. Often, R.sup.2 is seen as a measure of equivalence between the reference and evaluation methods, systems or products. Unfortunately, R.sup.2 is susceptible to a priori manipulation. For example, suppose two tests designed to measure cholesterol values in human blood are to be compared. Some patients may have very high cholesterol values while others may have very low cholesterol values. If two methods for measuring cholesterol are being compared using a linear regression best-fit line, then a high value of R.sup.2 may be falsely interpreted as indicating equivalence of the two methods. In fact, the high value of R.sup.2 is may only be indicating that there are patients included in the study whose cholesterol values are at the high and low ends of the human spectrum. Because R.sup.2 is susceptible to manipulation, it is not a good quantity to be depended upon for measuring the clinical equivalence of a new test method. 
         [0009]    Still another disadvantage of current test validation methods, is that they typically validate only a single test method at a time. Thus, for a testing device which is capable of testing  30  separate analytes, using previous testing validation methods  30  separate validations will have to be performed. Accordingly, it would be advantageous to have a single software package which could validate all 30 testing methods at one time. 
         [0010]    Therefore, there is a need for a test method validation system which reliably measures the accuracy and precision of a new testing method, determines whether the new testing method is clinically equivalent to a previous testing method, and is capable of validating a plurality of test methods at one time. 
       SUMMARY OF THE INVENTION 
       [0011]    The above needs are addressed and other advantages are realized in a method and system according to an embodiment of the present invention. The method according to an embodiment of the present invention comprises the steps of determining a level of variance in a reference method, determining the average difference in results of the reference and evaluation testing methods, and comparing the average difference between the two methods relative to the level of variability of the reference, and based on the comparison, generating a report indicating whether the evaluation testing method is clinically equivalent to the reference method. The acceptable difference between results of the reference and evaluation testing methods can be calculated by comparing two sets of reference test data associated with the reference method. Alternatively, the acceptable difference can be defined by the user. The report comprises a plot of confidence intervals for bias, modified mean difference plot, a variability chart having a first axis representing accuracy and a second axis representing precision, a scatter diagram with best-fit regression line and associated statistics, as well as a conclusion as to whether the evaluation testing method is clinically equivalent to the reference method. The report also contains a summary statistics table, a table of the bias confidence intervals, the limits on allowable bias as optionally input by the user, and an Appendix containing all the input data. Finally, in the method according to an embodiment of the present invention, data associated with the reference testing method and the evaluation testing method can be conveniently identified by the user through a graphical user interface. 
     
    
     
       BRIEF DESCRIPTION OF THE DRAWINGS 
         [0012]    The invention will be better understood with reference to the following description and the attached drawings, in which: 
           [0013]      FIG. 1  is a block diagram of a system according to an embodiment of the present invention; 
           [0014]      FIG. 2  is a screen shot representing a graphical user interface used to identify data in a spreadsheet representing reference and evaluation data in order to determine equivalence of testing methods; 
           [0015]      FIG. 3  is a flowchart illustrating a method according to an embodiment of the present invention; 
           [0016]      FIG. 4  is an optional output of the system, showing confidence intervals for two evaluation test methods; 
           [0017]      FIG. 5  is an optional output of the system, showing a mean difference plot for two evaluation test methods; 
           [0018]      FIG. 6  is a variability chart generated by the system, showing accuracy of an evaluated test method on the horizontal axis and precision of the evaluated test method on the vertical axis; 
           [0019]      FIGS. 7 and 8  are correlation plots generated by a system according to an embodiment of the invention, illustrating the correlation between observations obtained using the evaluated test method and observations obtained using the reference test method. 
       
    
    
       [0020]    In the drawing figures, it will be understood that like numerals refer to like structures and method steps. 
       DETAILED DESCRIPTION OF THE INVENTION 
       [0021]    A block diagram of an exemplary system  100  in accordance with an embodiment of the present invention is shown in  FIG. 1 . The system preferably includes a memory  102  for storing test data. The memory  102  is accessible from a processor  104 . Processor  104  receives inputs from input devices  106 , such as a keyboard and mouse. Processor  104  also produces outputs which are displayed on an output device  108 , which can be a monitor or printer, for instance. The memory  102  preferably stores test data to be evaluated, but may store other information, such as program instructions for executing a program in accordance with an embodiment of the present invention. Data can be entered into memory  102  through user input devices  106 , or alternatively, optional lab equipment  110  can automatically store test results. 
         [0022]    Processor  104  executes a set of machine instructions adapted to evaluate the test data stored in memory  102 . The test data relates to test results obtained using various testing methods on a common set of donors, as will be explained in greater detail below. The data includes at least one and preferably two results per subject using the reference (control) methods, and at least one result for each evaluation method. Processor  104  is adapted to perform a series of calculations which determine if the evaluation test methods are clinically equivalent to the reference method or methods. The calculations and steps performed by the processor to make this determination will be described in greater detail below. 
         [0023]    An exemplary set of data associated with two reference test method results and one result from each of two evaluation test methods per subject is reproduced in Appendix A. These data, as shown, are preferably stored in a spreadsheet program, such as Microsoft™. Excel. As shown, the data are stored in cells of a table identified by columns and rows. Rows 2-4 of the exemplary table contain information about the test, including the test name, the units appropriate to the results of each test, and user-defined limits of equivalence (acceptable bias) for each test. As shown the limits can be expressed in exact quantities, such as 2 mmol/L for Sodium, or in percentages, such as 10% for AST. 
         [0024]    As further shown in the table of Appendix A, Row 6 contains labels for f each of the columns of data in rows 7 and above. Column A contains donor numbers, column B contains the main variable in the testing methods (the blood collection tube type), Column C contains results of the tests for Sodium, Column D contains results of the tests for AST, and Column E contains results of the tests for Triglycerides. There were three types of blood collection tubes used in this study, Serum, SST.™., and SST II.™. As can further be observed from the exemplary table of Appendix A, specimens from 30 donors were tested, and each donor was tested for three analytes, Sodium, AST, and Triglycerides. For each donor, four blood specimens were drawn, two with the Serum type tube, and one each with the SST.™. and SST II.™. tubes, with each of the three analytes being measured in each specimen. Two specimens were drawn with the Serum tube, which in this case was considered to be the reference or control method. One specimen was drawn with each of the two evaluation devices. Thus there were twelve results (4 for each analyte) for each donor. 
         [0025]    Tube type is the main variable in the exemplary test methods, but it should be understood that any variable could be evaluated, and blood collection tube type is chosen and discussed herein simply as an example. The serum tube was the reference or control device. The first evaluation device in this example was a blood collection tube labeled SST.™., and the second evaluation device was a blood collection tube labeled SST II.™. 
         [0026]    The user interface will now be described in connection with  FIG. 2 , which is a screen shot of a user interface according to an embodiment of the invention. In the preferred embodiment of the invention, a graphical computer interface such as the one shown in  FIG. 2  is provided. The invention is embodied in a computer program which acts as a plug-in to Microsoft.®. Excel. Of course it will be understood by those of skill in the art that the invention could be programmed as an independent software application running on a personal computer, or embedded in hardware, or implemented in any other suitable manner. When the plug-in is activated, the user interface  200  shown in  FIG. 2  is presented. 
         [0027]    The user interface  200  allows for the user to identify parts of a table, such as the spread sheet shown in Appendix A, which are related to reference and evaluation test methods, and to choose certain available options for the type of evaluation to be performed, as well as the types of outputs desired. The user then uses a mouse or other suitable input device to identify the corresponding portions of the table which contain the information needed by the program to perform the necessary calculations and generate the desired output. 
         [0028]    For example, a portion of the user interface  200  is labeled “Study Information”  202 . This portion includes Experiment Name  204 , Analyte Names  206 , and Analyte Units  208 . The user has the option of typing the cell range corresponding to “Experiment Name” directly into the space provided for in the user interface at  204 , or to click a button  210  allowing the user to use a mouse to identify the corresponding cell range within the Excel worksheet. Since the Experiment Name in this example is “Anaplot Test” at cell A6 of the table in Appendix A, cell A6 would be identified by the user in field  204  of the user interface. Similarly, cells C6-E6 would be identified as corresponding to the “Analyte Names” at  206  of the user interface  200 . Cells C4-E4 would be identified as corresponding to “Analyte Units”  208  in the user interface  200 . 
         [0029]    A type of Mean Difference Limit Calculation is selected using the user interface  200  at  212 . The choices are Replicated Control Calculation  214 , Bland Altman  216 , Given Variability  218 , and No Control Limits  220 . Only one of the four selection can be selected. Also, a choice between Constant CV  222  and Constant SD  224  is provided in this section  212 . The types of Mean Difference Limit Calculations will be discussed in further detail below. 
         [0030]    A portion of the user interface  200  is provided to allow for the selection of desired outputs  226 . The possible selections preferably include Confidence Limits for Bias  228 , Mean Difference Plot  230 , Chevron Plot  232 , Correlation Plot  234 , and Data in Appendix  236 . A checkbox for each type of output to be included is provided, and selecting any of the output types will cause the output to be included in the report generated by the system. The Clinical Criteria for Bias Limits  238  can also be set, either by entering the criteria directly in the space provided, or by referring to cells in a table which contain the clinical criteria for bias limits, such as an Excel worksheet. 
         [0031]    A section of the interface  200  is provided for identifying certain relevant data  240 . The data identified in this section includes a Donor ID Column  242 , a Cont/Eval ID Column  244 , and a Data Range  246 . In the present example, Donor ID Column would refer to column A of the table reproduced in Appendix A. This is the column of data containing donor IDs. Cont/Eval ID Column  244  refers to the column in the table which contains the names of the reference and evaluation variables for each donor. In this example, column B of the table in Appendix A would be identified. Column B contains the labels for the blood collection tubes used in each test (Serum, SST.™., and SST II.™.). The data to be evaluated, including reference data and evaluation data as appropriate, are identified in the Data Range  246  field. In this example, columns C, D, and E are identified as corresponding to the test results for both the reference and evaluation tests. These columns contain the actual test data for the three analytes tested, and for each of the 30 donors. The interface  200  also includes a field for Control ID  248  and Evaluation ID  250 . A “Select All but Control” button  252  is provided. Finally, an “OK” button  254 , a “cancel” button  256 , an “add comparison” button  258  and a “restore prior values” button  260  are provided. 
         [0032]    The method according to an embodiment of the present invention will now be described in connection with the flowchart of  FIG. 3 . At step  300  a reference method is conducted. Observations from the reference method are recorded at  302 . The reference method forms the basis for comparison to the evaluation method. Preferably, the reference method is performed at least twice, and observations of both reference methods are recorded. In this manner, the variability between successive runs of the same method can be measured. At step  304 , the evaluation method is performed, and observations are recorded at  306 . Preferably, the observations are recorded into a table, such as a Microsoft.®. Excel worksheet, to facilitate accessing the data for calculations to be performed by the statistical analysis program. More than one evaluation method may be performed and recorded. Advantageously, according to an embodiment of the present invention, any number of evaluation methods can be evaluated simultaneously. 
         [0033]    At  308  the statistical analysis program is started. Preferably, this produces an interface as described above in connection with  FIG. 2 . Various data are identified in the user interface  200  at  310 . Preferable, the data identified in the user interface  200  include the donor ID&#39;s associated with the data, the Control/Evaluation IDs, and the columns of data for the tests performed. A sample table of data is provided at Appendix A. 
         [0034]    Also in the interface  200 , the types of mean difference limit calculations desired are selected  312 . The types available are Replicated Control Calculation  214 , Bland Altman  216 , Given Variability  218 , and No Control Limits  220 . Also to be selected are constant CV  222  or constant SD  224 . If Replicated Control Calculation  214  is selected, the statistical program calculated the acceptable variability in the evaluation data based on the variability between the at least two sets of reference data. Bland Altman  216  selects a Bland Altman mean difference calculation. Given Variability  218  allows the user to select the acceptable variability. Finally, No Control Limits  220  allows the user to select a set of calculations without control limits. 
         [0035]    At step  314 , the user selects the desired set of outputs to be generated. These selections are available at  226  of the user interface  200 . The user&#39;s choices comprise Confidence Limits for Bias  228 , Mean Difference Plot  230 , Chevron Plot  232 , Correlation Plot  234 , and Data in Appendix  236 . Examples of each type of data will be described in greater detail below. 
         [0036]    Once all data have been identified, and calculations and outputs have been selected, the user selects the “OK” button  254  at step  316  to begin the calculations selected. 
         [0037]    A series of equations appropriate to the various selections available to the user are shown at Appendices B and C. Appendix B shows the set of equations associated with determining the slope and intercept in a correlation plot  234 . Different equations are provided for different combinations of calculation type, and the kind and number of reference and evaluation data sets, as well as the type of variation selected. Appendix C shows the set of equations used to generate Chevron Plot data. The Chevron Plot will be described in greater detail below in connection with  FIG. 4 . 
         [0038]    At step  318 , the system determines based on statistical analysis, whether the evaluation data indicates that the evaluation method is clinically equivalent to the reference method or methods. Finally, at step  320  the selected outputs are generated, along with conclusions reporting whether the evaluation method is clinically equivalent or not. 
         [0039]    Various outputs will now be described. The outputs described were based on the sample data provided in the table of Appendix A. A complete sample report is reproduced in Appendix D, and this report includes each of the types of outputs to be described in the foregoing description, for each of the three analytes tested in the reference and evaluation methods shown in Appendix A. For brevity, the outputs will each be described once in connection with one of the three analytes, AST. 
         [0040]      FIG. 4  illustrates the Confidence Limits for Bias output, selected by checking Confidence Limits for Bias  228  in the user interface  200 . The output shown in  FIG. 4  corresponds to the analyte AST which was tested for each donor and for each reference and evaluation test method. The 95% confidence interval for bias gives a feasible range of possible values for the average bias or difference between results obtained using a reference method or device and an evaluation method or device. Thus, if the 95% confidence interval for bias in AST between SST.™. and serum tubes is (5%, 8%), then there is 95% confidence that the true difference is somewhere between 5% and 8%. The confidence interval for each of the evaluation methods, SST.™. and SST II.™., are shown to be well within the 10% limits designated, indicating equivalence between the evaluation and reference devices. 
         [0041]      FIG. 5  illustrates a mean difference plot generated by the program according to an embodiment of the present invention. Data for each of the evaluation methods, SST.™. and SST II.™., are plotted. Each point represents a difference between the result observed using the reference method and the result observed using the evaluation method. 
         [0042]      FIG. 6  illustrates a Chevron Plot generated by the program according to an embodiment of the present invention. The Chevron Plot is a measure of bias (accuracy) and precision. Each evaluation experiment is plotted. Evaluation methods with a combination of good accuracy, and good precision are preferred. Regions are designated as “Good”, “Satisfactory”, “Unsatisfactory” and “Poor” so that the user can easily see which classification applies to each of the evaluation methods. Of course, it will be understood that while the Chevron Plot is the preferred manner of presenting accuracy and precision data, any graphical or non-graphical method of presenting accuracy and precision data is considered to be within the scope of the present invention. 
         [0043]      FIGS. 7 and 8  illustrate correlation plots generated according to an embodiment of the present invention.  FIG. 7  correlates reference (Serum) results with the first evaluation method (SST.™.).  FIG. 8  correlates reference results with the second evaluation method (SST II.™.). Regression is performed on the data and a regression line is plotted. An ideal line with slope equal to 1 and intercept equal to zero is also produced for comparison. 
         [0044]    A sample report generated by the system according to an embodiment of the invention is reproduced in Appendix D. The report includes the various outputs selected in the user interface  200  as described above for each analyte tested. Also, the report includes conclusions about the clinical equivalence of the evaluation methods for each of the analytes evaluated. In this manner, new test methods (including existing test methods with new components, such as blood collection tubes, chemical reagents or analytical instruments), can be evaluated, and a lab can quickly and definitively determine that test results using the new method are clinically equivalent to previous test results. If the new method is shown not to be clinically equivalent, steps can be taken to correct the problem. 
         [0045]    While the invention has been described by means of specific embodiments and applications, numerous modifications or variations could be made thereto by those skilled in the art without departing from the scope of the invention as set forth in the appended claims and equivalents thereof.

Technology Category: 3