LIAISON® XL MUREX Anti-HBs, LIAISON® XL MUREX Control Anti-HBs and LIAISON® XL MUREX Anti-HBs Verifiers

{0} SUMMARY OF SAFETY AND EFFECTIVENESS DATA (SSED) I. GENERAL INFORMATION Device Generic Name: Antibody to Hepatitis B Surface Antigen (Anti-HBs assay) Device Trade Name: LIAISON® XL MUREX Anti-HBs LIAISON® XL MUREX Control Anti-HBs LIAISON® XL MUREX Anti-HBs Verifiers Device Procode: LOM Applicant’s Name and Address: DiaSorin Inc. 1951 Northwestern Avenue Stillwater, MN 55082 Date(s) of Panel Recommendation: None Premarket Approval Application (PMA) Number: P180039 Date of FDA Notice of Approval: February 21, 2020 II. INDICATIONS FOR USE The LIAISON XL MUREX Anti-HBs is an in vitro chemiluminescent immunoassay (CLIA) for the qualitative and quantitative determination of antibody to hepatitis B surface antigen (anti-HBs) in human adult and pediatric (2 – 21 years) serum and plasma (lithium and sodium heparin and K₂ EDTA) including separator tubes, on the LIAISON XL Analyzer. Assay results in conjunction with other hepatitis B virus (HBV) serological markers and clinical information may be used as an aid in the diagnosis of HBV infection in patients with symptoms of hepatitis or who may be at risk for HBV infection. The assay results may be used as an aid in the determination of susceptibility to HBV infection in individuals prior to or following HBV vaccination or where vaccination status is unknown. The assay is not approved for use in screening blood, plasma or tissue donors. The LIAISON XL MUREX Control Anti-HBs (negative and positive) is intended for use as assayed quality control samples to monitor the performance of the LIAISON XL MUREX Anti-HBs assay. The performance characteristics of LIAISON XL MUREX Control Anti-HBs have not been established for any other assays or instrument platforms. The LIAISON XL MUREX Anti-HBs Verifiers (level 1, 2, 3, and level 4) are assayed quality control materials intended for the quantitative verification of calibration and reportable range of the LIAISON XL MUREX Anti-HBs assay. The performance PMA P180039: FDA Summary of Safety and Effectiveness Data {1} characteristics of LIAISON XL MUREX Anti-HBs Verifiers have not been established in connection with any other assay or instrument platforms. ## III. CONTRAINDICATIONS There are no known contraindications. ## IV. WARNINGS AND PRECAUTIONS The warnings and precautions can be found in the LIAISON XL MUREX Anti-HBs labeling. ## V. DEVICE DESCRIPTION ### Kit Components **Reagents:** The LIAISON XL MUREX Anti-HBs is an *in vitro* diagnostic device consisting of four (4) reagents provided in individual compartments within a plastic container called the Reagent Integral. The assay configuration allows performance of 100 tests. The assay is comprised of the following components: - 1 vial of Magnetic particles coated with HBsAg obtained in mammalian cells by the recombinant DNA technology (balanced ad and ay subtypes), BSA, Phosphate buffer (PBS), &lt; 0.1% sodium azide. - 1 vial Calibrator 1 containing Human plasma containing low levels of anti-HBs fetal calf serum, EDTA and 0.2% ProClin® 300, preservatives. - 1 vial Calibrator 2 containing human plasma with high levels of anti-HBs fetal calf serum, EDTA. 0.2% ProClin® 300, preservatives, and an inert blue dye. - 1 vial Conjugate containing Heat-treated Human HBsAg (balanced ad and ay subtypes) conjugated to an isoluminol derivative, BSA, phosphate buffer (PBS), EDTA, 0.2% ProClin® 300, preservatives, and an inert blue dye. **Controls:** LIAISON XL MUREX Control Anti-HBs set consists of 2 levels (positive and negative) ready to use controls. Each control solution allows at least 20 tests to be performed. The control set is an additional material required to perform the test. The controls are comprised of the following components: - 2 vials of Negative control containing Human serum without anti-HBs antibodies with 0.2% ProClin® 300 and preservatives - 2 vials of Positive control containing Human plasma with anti-HBs antibodies, 0.2% ProClin® 300 and preservatives **Verifiers:** LIAISON XL MUREX Anti-HBs Verifier set consists of 4 levels (A-D) ready to use verifiers. Each verifier solution allows at least 20 tests to be performed. The Verifier set is an additional material required to perform the test. PMA P180039: FDA Summary of Safety and Effectiveness Data {2} The Verifiers are comprised of the following components: - 1 vial per level A to D, containing Human plasma with 4 different levels of anti-HBs, $0.2\mathrm{ProClin}^{\text{®}}$ and preservatives. In addition, the following Analyzer and accessories are required for performing the LIAISON XL MUREX Anti-HBs, LIAISON XL MUREX Control Anti-HBs and the LIAISON XL MUREX Anti-HBs Verifiers: - LIAISON XL Analyzer is a fully automated chemiluminescent analyzer, performing the complete sample processing steps of the chemiluminescent assay and interprets the results. - LIAISON Wash/System Liquid (10x) - phosphate buffer solution, $&lt; 0.1\%$ sodium azide. - LIAISON XL Starter Kit - catalyst in $4\%$ sodium hydroxide solution and $0.12\%$ hydrogen peroxide solution # Assay Principle The qualitative and quantitative determination of anti-HBs is a direct, sandwich chemiluminescence immunoassay (CLIA). Anti-HBs present in samples, calibrators, or controls binds to the solid phase and HBsAg conjugate, thus forming a sandwich. After the incubation, the unbound material is removed with a wash cycle. Subsequently, the starter reagents are added and a flash chemiluminescence reaction is thus induced. The light signal, and hence the amount of isoluminol-HBsAg conjugate, is measured by a photomultiplier as relative light units (RLU) and is indicative of anti-HBs concentration present in the sample. Table 1: Initial Interpretation of Results for the LIAISON XL MUREX Anti-HBs is as follows: | Initial Result LIAISON XL Anti-HBs assay | | | | --- | --- | --- | | mIU/mL | Results | Retest Procedure | | < 9.0 | Negative | No retest is required. | | 9.0 < x < 11.0 | Equivocal | Retest in duplicate with the LIAISON XL Anti-HBs assay. | | ≥ 11.0 | Positive | No retest is required. | PMA P180039: FDA Summary of Safety and Effectiveness Data {3} Table 2: Final Interpretation of Results for the LIAISON XL MUREX Anti-HBs is as follows: | Final Result LIAISON XL Anti-HBs assay | | | | --- | --- | --- | | Result After Retest | Final Result | Clinical Interpretation of the Final Results | | Both retest results are <10 IU/mL | Negative | Anti-HBs concentration detected at < 10 mIU/mL. Individual is considered to be not immune to infection with HBV. | | 2 results out of 3 <10 IU/mL | Negative | Anti-HBs concentration detected at < 10 mIU/mL. Individual is considered to be not immune to infection with HBV. | | 2 results out of 3 ≥10 IU/mL | Positive | Anti-HBs concentration detected at ≥ 10 mIU/mL. Individual is considered to be immune to infection with HBV. | | Both retest results are ≥10 IU/mL | Positive | Anti-HBs concentration detected at ≥ 10 mIU/mL. Individual is considered to be immune to infection with HBV. | VI. ALTERNATIVE PRACTICES AND PROCEDURES There are several other alternatives for the detection and quantitation of antibodies to hepatitis B surface antigen (Anti-HBs). There are currently several FDA approved in vitro diagnostic tests commercially available for serological markers of hepatitis B virus (HBV) infection which, when used in conjunction with a patient's medical history, clinical examination and other laboratory findings, may be used as an aid in the diagnosis of HBV infection in patients with symptoms of hepatitis or who may be at risk for HBV infection. The assay may be used as an aid in the determination of susceptibility to hepatitis B virus (HBV) infection in individuals prior to or following HBV vaccination or where vaccination status is unknown. Each alternative has its own advantages and disadvantages. A patient should fully discuss these alternatives with his/her physician to select the method that best meets expectations and lifestyle. VII. MARKETING HISTORY The LIAISON XL MUREX Anti-HBs assay (318220) and LIAISON XL MUREX Control Anti-HBs (318221) are essentially the same as the CE-marked LIAISON XL murex Anti-HBs assay (311220) and LIAISON XL murex Control Anti-HBs (311221) with some minor modifications to raw material manufacturing processes. The LIAISON XL MUREX Anti-HBs assay (318220), LIAISON XL MUREX Control Anti-HBs (318221) and the LIAISON XL MUREX Anti-HBs Verifiers (318223) have not been marketed in the U.S. or any foreign country. The CE-marked LIAISON XL murex Anti-HBs assay (311220) and LIAISON XL murex Control Anti-HBs (311221) have been marketed in multiple countries. These devices PMA P180039: FDA Summary of Safety and Effectiveness Data {4} have not been withdrawn from the market in any country for reasons relating to safety and effectiveness. The following table includes a list all countries where the CE-marked versions have been marketed in the past year. Table 3: Countries where CE Marked LIAISON XL murex Anti-HBs (311220) and LIAISON XL murex Control Anti-HBs (311221) is sold | Austria | Australia | Bangladesh | | --- | --- | --- | | Belgium | Bulgaria | Brunei | | Brazil | Bahamas | Switzerland | | Chile | Colombia | Cyprus | | Czech Republic | Germany | Denmark | | Dominican Republic | Egypt | Spain | | Finland | France | United Kingdom | | Greece | Croatia | Hungary | | Ireland | Israel | Iraq | | Iran | Italy | Kuwait | | Lebanon | Luxembourg | Morocco | | Netherlands | Norway | Perù | | Poland | Portugal | Paraguay | | Romania | Saudi Arabia | Slovenia | | Thailand | Tunisia | Turkey | | South Africa | | | ## VIII. POTENTIAL ADVERSE EFFECTS OF THE DEVICE ON HEALTH Below is a list of the potential adverse effects (e.g., complications) associated with the use of the device. The LIAISON XL MUREX Anti-HBs is intended for *in vitro* diagnostic use, and as a result, there is no direct adverse effect on the patient. Standard good laboratory practices are considered sufficient to minimize risks to the end user. Failure of the product to perform as intended or human error in the use of the test may lead to a false result. Appropriate Warnings and Precautions for identified risks are contained in the labeling and assay Instructions for Use. A false positive result in a diagnostic setting includes improper patient management, including treatment for hepatitis B with antiviral medication. Antiviral medical has risks including toxicity and more rarely allergic reactions. Over time, viral resistance in patients who are co-infected but undiagnosed with other viruses using the same antiviral medication, such as HIV, can lead to viral resistance; however, the chance of an undiagnosed co-infection in a patient tested for hepatitis B is exceedingly unlikely. PMA P180039: FDA Summary of Safety and Effectiveness Data Page 5 {5} Furthermore, a false positive result when the device is used as an aid in the determination of susceptibility to HBV infection in individuals prior to or following HBV vaccination or where vaccination status is unknown includes leading a provider to falsely believe that a patient has been vaccinated in the past and/or has current immunity when the patient does not. This could lead to a patient inappropriately missing a vaccination. Additionally and likely more importantly, because hepatitis B surface antibody is ordered as part of a panel in clinical practice, this risk will likely be mitigated as incongruous test results would lead a clinician to either retest the patient or further investigate the etiology of hepatitis. As the performance of the assay in the clinical trial suggests that false positive results will be uncommon, the true risk of a false negative is likely minimal. A false negative result when the device is used as an aid in the determination of susceptibility to HBV infection in individuals prior to or following HBV vaccination or where vaccination status is unknown include potentially missing and undertreating a patient who has hepatitis B infection and whose clinical picture warrants antiviral treatment. Again, because hepatitis B surface antibody is ordered as part of a panel in clinical practice, the risk of missing and undertreating a patient who has hepatitis B infection will likely be mitigated as incongruous test results would lead a clinician to either retest the patient or further investigate the etiology of hepatitis. As the performance of the assay in the clinical trial suggests that false negative results will be uncommon, the true risk of a false negative is likely minimal. For the specific adverse events that occurred in the clinical study, please see Section X below. ## IX. SUMMARY OF NONCLINICAL STUDIES ### A. Laboratory Studies #### 1. Cut-off Determination The cut-off was established internally at DiaSorin and verified by testing a total of 113 samples (55 known negative and 58 known positive). A Receiver Operating Characteristics (ROC) analysis was performed on the results of the specimens tested. The assay's cut-off was evaluated with the observed results to demonstrate that its selection represents the best level of specificity, without compromising the sensitivity. The cut-off value at $10.0\mathrm{mIU/mL}$ is within the optimal range determined by the ROC curve to discriminate between negative and positive results. The established cut-off Index is $10.0\mathrm{mIU/mL}$, with an equivocal range of $\pm 10\%$ (9.00 - 11.0 mIU/mL). PMA P180039: FDA Summary of Safety and Effectiveness Data Page 6 {6} 2. Sensitivity / Seroconversion Panels The seroconversion sensitivity of the LIAISON XL MUREX Anti-HBs assay has been demonstrated by testing 10 commercial seroconversion panels in comparison to a reference anti-HBs immunoassay in terms of number of days from initial draw to first positive sample, as well as the difference between the last negative results and the first positive results. The LIAISON XL MUREX Anti-HBs assay yielded a positive result sooner by one blood draw or more than the comparator assay in the 10 panels. 3. Analytical Sensitivity / Dilution Study with Standard The sensitivity of the LIAISON XL MUREX Anti-HBs assay was evaluated by preparing serial dilutions of the WHO Second International Standard for anti-hepatitis B surface antigen (anti-HBs) immunoglobulin, human NIBSC code 07/164 in serum and plasma negative anti-HBs. Dilutions were tested in five (5) replicates on one (1) kit lot and on one (1) LIAISON XL Analyzer. The LIAISON XL MUREX Anti-HBs assay demonstrated linearity and accuracy between 3 and 500 mIU/ml. 4. Endogenous Interference The LIAISON XL MUREX Anti-HBs assay was tested for potential interference of high levels of endogenous substances including Triglycerides (3000 mg/dL), Hemoglobin (1000 mg/dL), Bilirubin (conjugated and unconjugated 20 mg/dL), Albumin (6000 mg/dL) and Cholesterol (350 mg/dL). Ten (10) negative samples or negative pools were spiked with an IgG anti-HBs high positive sample to achieve high negative, low positive and moderate samples. Samples were tested in 26 replicates each on one (1) kit lot. No interference was observed at the levels tested. 5. Analytical Specificity (Cross-Reactivity) A study was conducted to evaluate the LIAISON XL MUREX Anti-HBs assay for cross-reactivity with specimens from individuals with medical conditions unrelated to HBV infection. A total of 301 samples from 28 unrelated medical conditions were tested in singlicate on one (1) kit lot of LIAISON XL MUREX Anti-HBs and on a reference Anti-HBs assay. Of the 301 samples, no evidence of cross-reactivity was observed. The results of each potential cross-reactant are shown in in table below. PMA P180039: FDA Summary of Safety and Effectiveness Data Page 7 {7} Table 4: Summary of Cross-Reactivity Testing | | | N° of observed negative results | | | --- | --- | --- | --- | | Potential cross reactant | N° of expected negative samples | LIAISON XL MUREX Anti HBs | Reference Method | | Anti-nuclear antibodies (ANA) | 10 | 10 | 10 | | Auto-immune hepatitis | 10 | 10 | 10 | | C. trachomatis | 11 | 11 | 11 | | CMV (anti-CMV IgG or IgM positive) | 11 | 11 | 11 | | EBV (IgM positive) | 11 | 11 | 11 | | Fatty liver disease | 11 | 11 | 11 | | HAMA | 11 | 11 | 11 | | Hemodialysis patient | 11 | 11 | 11 | | Hepatitis A Virus (IgM positive) | 11 | 11 | 11 | | Hepatitis C Virus (anti-HCV ) | 11 | 11 | 11 | | Hepatocellular carcinoma | 11 | 11 | 11 | | HIV-1 (anti-HIV-1 positive) | 11 | 11 | 11 | | HIV-2 (anti-HIV-2 positive) | 11 | 11 | 11 | | HSV (anti-HSV IgG or IgM positive) | 11 | 11 | 11 | | HTLV-1/2 (anti-HTLV positive) | 11 | 11 | 11 | | IgG monoclonal gammopathy | 11 | 11 | 11 | | IgM monoclonal gammopathy | 10 | 10 | 10 | | Influenza vaccine recipients | 11 | 11 | 11 | | Multiparous pregnancies | 10 | 10 | 10 | | Multiple myeloma | 11 | 11 | 11 | | Multiple transfusion recipients | 10 | 10 | 10 | | N. gonorrhoea | 11 | 11 | 11 | | Pregnancy 1sttrimester | 10 | 10 | 10 | | Pregnancy 2ndtrimester | 10 | 10 | 10 | | Pregnancy 3rdtrimester | 11 | 11 | 11 | | Rheumatoid Factor | 11 | 11 | 11 | | T. pallidum (anti-T. pallidum IgG and/or IgM positive) | 11 | 11 | 11 | | T.cruzi (anti-T. cruzi positive) | 11 | 11 | 11 | # 6. Sample Equivalence/Matrix Effect Twenty-five (25) paired sets of matched serum (with and without gel SST) and plasma (lithium and sodium heparin and $\mathrm{K}_2\mathrm{EDTA}$ ) were tested to determine if these sample types provide equivalent results on the LIAISON XL MUREX Anti-HBs assay. Each sample was divided into three aliquots. Two sets of aliquots were spiked with an anti-HBs high positive sample to achieve two (2) levels of samples: high negative and low positive samples. The third set of aliquots was un-spiked to serve as control samples. The results of the negative and low positive samples did not change the classification of the expected result. PMA P180039: FDA Summary of Safety and Effectiveness Data {8} The results obtained on the serum-plasma paired samples indicate that there is equivalence among serum (with and without Gel SST), $\mathrm{K}_2$ -EDTA, Lithium Heparin and Sodium Heparin plasma, as indicate in the table below: | Sample Type | Slope | Intercept | | --- | --- | --- | | Serum with Gel separator | 0.987 | 0.138 | | K2-EDTA | 0.971 | -0.036 | | Lithium Heparin | 1.023 | -0.150 | | Sodium Heparin | 0.998 | -0.099 | # 7. Carry-Over Study The LIAISON XL Analyzer uses disposable tips for sample pipetting. A carry-over study was performed to evaluate the extent of carryover and the associated residual risk for signal carryover in the instrument's measuring cell as the result of a high signal-generating sample. Two samples were used for this evaluation: one (1) anti-HBs negative human serum sample and one (1) human positive sample/pool with a high level of anti-HBs analyte. The samples were tested in singlicate in five (5) runs in the following sequence: High Pos, Neg, High Pos, Neg, High Pos, Neg, High Pos, Neg, High Pos, Neg. All acceptance criteria were met, demonstrating that no significant amount of analyte is carried over from one sample reaction into the subsequent sample reactions. # 8. Stability Studies # Sample Stability Studies were performed to determine the storage stability of patient serum and plasma samples at storage temperatures of $2 - 8^{\circ}\mathrm{C}$ , room temperature (RT), $-20^{\circ}\mathrm{C}$ . A multiple freeze/thaw (F/T) study was also performed. Serum and plasma samples tested contained Anti-HBs analyte levels of negative, high negative and low positive. $2 - 8^{\circ}\mathrm{C}$ study - samples were tested unstressed $(\mathrm{T} = 0)$ , and again after 1, 2, 3, 4, 5, 7 and 8 days of storage at $2 - 8^{\circ}\mathrm{C}$ for 24 hours per day. &gt; room temperature study (RT) - samples were tested immediately after preparation and again after 1, 2, 3, 4, and 5 days of storage at RT for 24 hours each day. - $20^{\circ}\mathrm{C}$ study - samples were tested unstressed $(\mathrm{T} = 0)$ and stored at $-20^{\circ}\mathrm{C}$ or lower for 1, 3, and 4 months. &gt; Freeze/Thaw (F/T) study - samples were tested unstressed $(\mathrm{T} = 0)$ and after 1, 2, 3, 4, 5, 6, and 7 F/T cycles. Samples were frozen for 12-24 hours at $-20^{\circ}\mathrm{C}$ or lower and thawed at room temperature. PMA P180039: FDA Summary of Safety and Effectiveness Data {9} The results of the studies indicate serum and plasma samples are stable for: | | Sample Stability Claims | | | | | --- | --- | --- | --- | --- | | Sample Matrix | Number of Freeze and Thaw Cycles | Storage at 2-8°C | Storage at -20°C | Storage at Room Temperature | | Serum | 6 | 7 days | 3 months | 1 day | | Plasma | 1 | 7 days | 3 months | 1 day | ## Reagent Stability ### Real-Time (Shelf-Life) Studies were performed to establish the shelf-life for the LIAISON XL MUREX Anti-HBs assay. Three (3) lots of LIAISON XL MUREX Anti-HBs were stored at the recommended storage temperature of 2-8°C throughout the study. Performance was assessed against clinically relevant acceptance criteria using three (3) lots LIAISON XL MUREX Control Anti-HBs (positive and negative) and an internal stability panel consisting of eight (8) samples. Study results demonstrate that reagents are stable and continue to meet acceptance criteria ten (10) months after the date of manufacture for the LIAISON XL MUREX Anti-HBs. ### Reagent On-Board Stability studies were conducted to determine the length of time the LIAISON XL MUREX Anti-HBs Reagent Integral can be stored on-board the LIAISON XL Analyzer in the refrigerated area once opened. One (1) lot of the LIAISON XL MUREX Anti-HBs assay was stored on-board the LIAISON XL Analyzer throughout the 13 weeks of the study. The LIAISON XL MUREX Control Anti-HBs (negative and positive) along with the internal stability panel were tested in duplicate at one (1) week intervals up to the 13 weeks. The LIAISON XL MUREX Anti-HBs assay is stable on-board the LIAISON XL Analyzer for 6 weeks. ### Reagent Open Use The aim of this study was to assess the open use stability of the LIAISON XL MUREX Anti-HBs kit reagents by simulating normal conditions of use as specified in the instruction for use. Testing of samples was performed in duplicate, on one (1) lot of LIAISON XL MUREX Anti-HBs and one (1) lot of LIAISON XL MUREX Control Anti-HBs. Results were calculated using the initial (time zero) assay calibration. PMA P180039: FDA Summary of Safety and Effectiveness Data Page 10 {10} The opened Reagent Integral was then removed from the XL Analyzer and stored at 2-8 °C. Kit performance using the opened Reagent Integral was evaluated weekly up to 13 weeks. The Reagent Integral is stable after opening for 6 weeks when stored at 2-8 °C. ## Temperature Stress/Reagent Transport Study The transport simulation tests were performed in order to verify that kit reagents maintain their properties during the shipment and delivery conditions to the customer. After being subjected to simulated stress conditions, testing was performed on 1 lot of LIAISON XL MUREX Anti-HBs at midlife and will be tested at expiration. All testing performed meets acceptance criteria under various simulated transport conditions. ## Calibrator Stability The LIAISON XL MUREX Anti-HBs calibrators are included on the Reagent Integral. All studies for the Reagent Integral are applicable to the 2 levels of calibrators provided. ## Calibration Interval Stability The aim of this study was to assess stability of the product calibration by simulating normal condition of use as specified in the instruction for use. A calibration was performed at time 0 and the Reagent Integral was stored on board the analyzer for the duration of the study. Kit performance was evaluated weekly up to nine (9) weeks by testing the stability panel and LIAISON XL MUREX Control Anti-HBs on one (1) lot of LIAISON XL MUREX Anti-HBs reagents. Results were generated using the initial (time zero) assay calibration and performance was assessed against clinically relevant acceptance criteria. Results demonstrate that the LIAISON XL MUREX Anti-HBs calibration is stable for six (6) weeks. ## Control stability ### Real-time (Shelf-Life) Studies were performed to establish the shelf-life for the LIAISON XL MUREX Control Anti-HBs and the LIAISON XL MUREX Anti-HBs Verifiers. Three lots of LIAISON XL MUREX Control Anti-HBs were stored at the recommended storage temperature of 2-8°C throughout the study. PMA P180039: FDA Summary of Safety and Effectiveness Data Page 11 {11} Current results demonstrate that the positive and negative controls are stable and continue to meet acceptance criteria at eighteen (18) months. ## Open use The aim of this study was to assess stability of the opened Control vials by simulating normal conditions of use, as specified in the instruction for use. Testing was performed in duplicate, on one lot of LIAISON XL MUREX Control Anti-HBs. LIAISON XL MUREX Control Anti-HBs (negative and positive) were within their established ranges and were assessed against clinically relevant acceptance criteria. The LIAISON XL MUREX Control Anti-HBs (negative and positive) are stable for 6 weeks after opening when stored at 2-8 °C between uses. ## Temperature Stress/Reagent Transport Study The transport simulation tests were performed in order to ensure that kit Controls maintain their properties during the shipment and delivery conditions to the customer. After being subjected to simulated stress conditions testing was performed on 1 lot of LIAISON XL MUREX Control Anti-HBs. All testing performed meets acceptance criteria under various simulated transport conditions. ## 9. Precision ### Internal 20 Days A precision/reproducibility study was carried out over a period of twenty (20) days on the LIAISON XL MUREX Anti-HBs assay using the LIAISON XL Analyzer. The CLSI document EP05-A3 was consulted in the preparation of the testing protocol. The testing was performed internally at DiaSorin S.p.A. A coded panel of eight (8) serum-based samples consisting of 1 Negative, 1 High Negative, 1 Low Positive, 1 Moderate Positive and 4 Positive along with 3 lots of the LIAISON XL MUREX Control Anti-HBs (neg and pos) and 3 lots of the LIAISON XL MUREX Anti-HBs Verifiers were tested in 2 replicates per run, 2 runs per day for 20 days using 3 different LIAISON XL MUREX Anti-HBs assay reagents and spanning at least 2 calibration cycles. The Repeatability of the combined 3 lots of LIAISON XL MUREX Anti-HBs ranged from 1.3% to 3.1%. The with-in Laboratory %CV of the combined 3 lots of LIAISON XL MUREX Anti-HBsc ranged from 4.2% to 15.1%. The results are shown below. PMA P180039: FDA Summary of Safety and Effectiveness Data Page 12 {12} Table 5: Summary of Precision Study | LIAISON XL MUREX Anti-HBs Assay All 3 Lots Combined | | | | | | | | | | | | | --- | --- | --- | --- | --- | --- | --- | --- | --- | --- | --- | --- | | Sample ID | N | Mean | Repeatability | | Between-Run | | Between-Day | | Between-Lot | | Within Laboratory | | | | | SD | %CV | SD | %CV | SD | %CV | SD | %CV | SD | | Ctrl Neg #RS-764 | 240 | *977 | 32.198 | 3.3% | 7.269 | 0.7% | 24.653 | 2.5% | 20.068 | 2.1% | 45.826 | | Ctrl Neg #RS-765 | 240 | *940 | 27.365 | 2.9% | 13.132 | 1.4% | 18.266 | 1.9% | 17.476 | 1.9% | 39.501 | | Ctrl Neg #RS-766 | 240 | *941 | 25.578 | 2.7% | 17.607 | 1.9% | 19.764 | 2.1% | 20.353 | 2.2% | 42.061 | | Ctrl Pos #RS-767 | 240 | 51.9 | 0.825 | 1.6% | 0.905 | 1.7% | 0.694 | 1.3% | 5.428 | 10.5% | 5.608 | | Ctrl Pos #RS-768 | 240 | 56.4 | 0.908 | 1.6% | 1.012 | 1.8% | 0.641 | 1.1% | 4.215 | 7.5% | 4.475 | | Ctrl Pos #RS-769 | 240 | 53.7 | 0.890 | 1.7% | 1.169 | 2.2% | 0.578 | 1.1% | 3.967 | 7.4% | 4.269 | | Cal Ver #RS-784 A | 240 | 7.56 | 0.236 | 3.1% | 0.154 | 2.0% | 0.181 | 2.4% | 0.95 | 12.6% | 1.007 | | Cal Ver #RS-784 B | 240 | 20.1 | 0.396 | 2.0% | 0.248 | 1.2% | 0.364 | 1.8% | 2.47 | 12.3% | 2.54 | | Cal Ver #RS-784 C | 240 | 72.6 | 1.022 | 1.4% | 0.681 | 0.9% | 0.857 | 1.2% | 6.809 | 9.4% | 6.972 | | Cal Ver #RS-784 D | 240 | 237 | 2.973 | 1.3% | 3.572 | 1.5% | 2.681 | 1.1% | 27.599 | 11.6% | 28.116 | | Cal Ver #RS-785 A | 240 | 6.94 | 0.214 | 3.1% | 0.103 | 1.5% | 0.146 | 2.1% | 0.658 | 9.5% | 0.715 | | Cal Ver #RS-785 B | 240 | 18.3 | 0.412 | 2.3% | 0.339 | 1.9% | 0.375 | 2.1% | 1.662 | 9.1% | 1.786 | | Cal Ver #RS-785 C | 240 | 75.1 | 0.870 | 1.2% | 1.042 | 1.4% | 0.885 | 1.2% | 4.376 | 5.8% | 4.666 | | Cal Ver #RS-785 D | 240 | 238 | 3.747 | 1.6% | 2.507 | 1.1% | 3.324 | 1.4% | 19.32 | 8.1% | 20.116 | | Cal Ver #RS-786 A | 240 | 7.15 | 0.223 | 3.1% | 0.080 | 1.1% | 0.203 | 2.8% | 0.7 | 9.8% | 0.767 | | Cal Ver #RS-786 B | 240 | 19.4 | 0.371 | 1.9% | 0.371 | 1.9% | 0.289 | 1.5% | 1.736 | 8.9% | 1.836 | | Cal Ver #RS-786 C | 240 | 77.3 | 1.038 | 1.3% | 0.935 | 1.2% | 1.122 | 1.5% | 5.436 | 7.0% | 5.723 | | Cal Ver #RS-786 D | 240 | 251 | 4.106 | 1.6% | 2.782 | 1.1% | 3.584 | 1.4% | 23.625 | 9.4% | 24.404 | | AHBS-1-U1 | 240 | *1024 | 27.177 | 2.7% | 18.492 | 1.8% | 18.060 | 1.8% | 22.522 | 2.2% | 43.749 | | AHBS-1-U2 | 240 | 7.32 | 0.205 | 2.8% | 0.124 | 1.7% | 0.135 | 1.8% | 1.116 | 15.3% | 1.149 | | AHBS-1-U3 | 240 | 16.9 | 0.386 | 2.3% | 0.618 | 3.7% | 0.000 | 0.0% | 1.841 | 10.9% | 1.98 | | AHBS-1-U4 | 240 | 26.9 | 0.457 | 1.7% | 0.405 | 1.5% | 0.556 | 2.1% | 3.967 | 14.8% | 4.052 | | AHBS-1-U5 | 240 | 35.2 | 0.608 | 1.7% | 0.675 | 1.9% | 0.313 | 0.9% | 2.234 | 6.4% | 2.432 | | AHBS-1-U6 | 240 | 76 | 1.385 | 1.8% | 0.410 | 0.5% | 1.062 | 1.4% | 4.744 | 6.2% | 5.071 | | AHBS-1-U7 | 240 | 122 | 1.770 | 1.4% | 1.288 | 1.1% | 1.693 | 1.4% | 14.523 | 11.9% | 14.784 | | AHBS-1-U8 | 240 | 289 | 4.745 | 1.6% | 5.408 | 1.9% | 3.250 | 1.1% | 38.677 | 13.4% | 39.475 | PMA P180039: FDA Summary of Safety and Effectiveness Data {13} # External Precision 5-day Study A five (5) day precision/reproducibility study was conducted at two (2) external laboratories and at DiaSorin Inc. to verify the precision of the LIAISON® XL MUREX Anti-HBs assay. The CLSI document EP15-A3 was consulted in the preparation of the testing protocol. The coded panel, comprised of eight (8) frozen serum samples was the same panel used in the 20-day precision study. The precision panel was tested at all three (3) sites on the LIAISON® XL Analyzer using six (6) replicates per run in one (1) run per day for five (5) operating days with multiple technicians performing the testing. Table 6: Summary of Reproducibility Study | LIAISON XL MUREX Anti-HBs Assay All 3 Lots Combined | | | | | | | | | | | | | | --- | --- | --- | --- | --- | --- | --- | --- | --- | --- | --- | --- | --- | | Sample ID | N | Mean | Repeatability | | Between-Day/Run | | Within Laboratory Precision | | Between-sites/Lot | | Reproducibility | | | | | | SD | %CV | SD | %CV | SD | %CV | SD | %CV | SD | %CV | | Ctrl Neg (All 3 lots) | 90 | 780.611 | 28.577 | 3.7% | 13.741 | 1.8% | 31.710 | 4.1% | 51.133 | 6.6% | 60.167 | 7.7% | | Ctrl Pos (All 3 lots) | 90 | 53.777 | 1.313 | 2.4% | 0.811 | 1.5% | 1.543 | 2.9% | 1.862 | 3.5% | 2.418 | 4.5% | | Cal Ver A (All 3 lots) | 90 | 7.278 | 0.217 | 3.0% | 0.082 | 1.1% | 0.232 | 3.2% | 0.227 | 3.1% | 0.325 | 4.5% | | Cal Ver B (All 3 lots) | 90 | 19.269 | 0.527 | 2.7% | 0.279 | 1.4% | 0.596 | 3.1% | 1.044 | 5.4% | 1.202 | 6.2% | | Cal Ver C (All 3 lots) | 90 | 74.560 | 1.345 | 1.8% | 1.253 | 1.7% | 1.838 | 2.5% | 1.200 | 1.6% | 2.195 | 2.9% | | Cal Ver D (All 3 lots) | 90 | 242.422 | 4.881 | 2.0% | 3.828 | 1.6% | 6.203 | 2.6% | 13.707 | 5.7% | 15.045 | 6.2% | | AHBS-1-U1 | 90 | 847.011 | 22.506 | 2.7% | 14.415 | 1.7% | 26.727 | 3.2% | 54.888 | 6.5% | 61.049 | 7.2% | | AHBS-1-U2 | 90 | 7.119 | 0.260 | 3.6% | 0.248 | 3.5% | 0.359 | 5.0% | 0.264 | 3.7% | 0.445 | 6.3% | | AHBS-1-U3 | 90 | 16.532 | 0.531 | 3.2% | 1.198 | 7.2% | 1.311 | 7.9% | 0.892 | 5.4% | 1.585 | 9.6% | | AHBS-1-U4 | 90 | 25.670 | 1.265 | 4.9% | 2.254 | 8.8% | 2.585 | 10.1% | 0.981 | 3.8% | 2.765 | 10.8% | | AHBS-1-U5 | 90 | 33.063 | 1.140 | 3.4% | 2.018 | 6.1% | 2.317 | 7.0% | 1.000 | 3.0% | 2.524 | 7.6% | | AHBS-1-U6 | 90 | 72.782 | 2.392 | 3.3% | 4.628 | 6.4% | 5.210 | 7.2% | 2.950 | 4.1% | 5.987 | 8.2% | | AHBS-1-U7 | 90 | 113.361 | 4.672 | 4.1% | 8.672 | 7.7% | 9.850 | 8.7% | 8.769 | 7.7% | 13.188 | 11.6% | | AHBS-1-U8 | 90 | 282.244 | 8.281 | 2.9% | 10.400 | 3.7% | 13.294 | 4.7% | 20.494 | 7.3% | 24.429 | 8.7% | *Precision calculations are based on signal (RLU) # 10. Pediatric and Adult Sample Equivalency Pediatric samples were tested to determine if these types of samples provide equivalent results to adult human serum. PMA P180039: FDA Summary of Safety and Effectiveness Data {14} A total of thirty (30) negative pediatric patient samples were used for this study. The pediatric samples encompassed the age range of two (2) months to twenty-one (21) years. Ten (10) pediatric samples were spiked with an anti-HBs high positive sample to obtain high negative samples. Ten (10) pediatric samples were spiked with an IgG anti-HBs high positive sample to obtain low positive samples. Ten (10) pediatric samples were spiked with an anti-HBs high positive sample to obtain moderate positive samples. Adult negative pool samples were used as controls and were spiked with an anti-HBs high positive sample to achieve the same three (3) levels of samples: high negative, low positive and moderate positive samples. The samples were tested in duplicate, with the LIAISON XL MUREX Anti-HBs assay. Percent (%) recovery of the analyte from the pediatric and adult blood was calculated for each sample. All acceptance criteria were met demonstrating acceptable performance of pediatric samples. It can be concluded that pediatric samples react in the same way as the adult samples and are acceptable for use in the LIAISON XL MUREX Anti-HBs assay. ## B. Animal Studies Not Applicable. ## C. Additional Studies Not Applicable. ## X. SUMMARY OF PRIMARY CLINICAL STUDY(IES) The applicant performed a clinical study to establish a reasonable assurance of safety and effectiveness for the detection and quantitation of antibodies to hepatitis-B surface antigen with the LIAISON XL MUREX Anti-HBs using samples that would routinely be tested for hepatitis in the US. Data from this clinical study were the basis for the PMA approval decision. A summary of the clinical study is presented below. ## A. Study Design A multi-site clinical agreement study was conducted to evaluate the clinical performance of the LIAISON XL MUREX Anti-HBs assay on samples that would routinely be tested for hepatitis and samples that were selected from individuals that were diagnosed with acute or chronic Hepatitis B infection. The clinical agreement study involved the testing of 3,082 samples on six (6) FDA approved reference assays, each detecting a unique serological marker (HBsAg, HBeAg, Anti-HBs, Anti-HBc, Anti-HBc IgM, and Anti-HBe) in order to determine the HBV classification for each of the samples tested. PMA P180039: FDA Summary of Safety and Effectiveness Data Page 15 {15} The samples were collected from 6 different countries: Russia, Colombia, Cameroon, Ghana, Nigeria, and the United States. The U.S. samples were from multiple states including Ohio, Pennsylvania, Indiana, Florida, California, Texas, New Jersey, Tennessee, Massachusetts, and Puerto Rico. The prospective (unselected) subjects were defined as follows: - Pediatric and adult male (38.2%), female (61.7%) and unknown gender (0.1%) subjects at risk for hepatitis due to medical conditions (dialysis, transplantation), occupation, lifestyle, behavior or a known exposure event. - Subjects showing signs or symptoms and individuals living in an area with a higher probability of HBV infection. - The demographic breakdown of the prospective population was as follows: American Indian/Alaskan Native (0.1%), Asian (0.8%), Black/African American (31.2%), Caucasian (62.5%), Other (5.2%), and Unknown (0.2%) with an age range of 2 - 98 years of age. The retrospective (selected/archived) samples were from male (69.5%), female (21.9%), and unknown gender (8.6%) subjects diagnosed with acute and/or chronic Hepatitis having an age range of 17 - 67 years of age from the following ethnicities: Asian (1.6%), Black/African American (23.8%), Caucasian (73%), other (1.2%) and 0.4% Unknown. The distribution of LIAISON XL MUREX Anti-HBs reactive and non-reactive results by age and gender of the overall prospective population are presented below. Table 7: Demographic Summary of the Prospective Population | Age Range | Gender | LIAISON XL MUREX | | | | | | --- | --- | --- | --- | --- | --- | --- | | | | + | | - | | Total | | | | n | % | n | % | | | 0-9 | F | 5 | 100.0% | 0 | 0.0% | 5 | | | M | 3 | 30.0% | 7 | 70.0% | 10 | | 10-19 | F | 21 | 52.5% | 19 | 47.5% | 40 | | | M | 8 | 53.3% | 7 | 46.7% | 15 | | 20-29 | F | 251 | 64.5% | 138 | 35.5% | 389 | | | M | 130 | 55.8% | 103 | 44.2% | 233 | | 30-39 | F | 253 | 53.4% | 221 | 46.6% | 474 | | | M | 111 | 49.6% | 113 | 50.4% | 224 | | 40-49 | F | 121 | 41.7% | 169 | 58.3% | 290 | | | M | 68 | 33.8% | 133 | 66.2% | 201 | | 50-59 | F | 106 | 45.7% | 126 | 54.3% | 232 | | | M | 70 | 37.8% | 115 | 62.2% | 185 | | 60-69 | F | 62 | 39.2% | 96 | 60.8% | 158 | | | M | 50 | 46.3% | 58 | 53.7% | 108 | PMA P180039: FDA Summary of Safety and Effectiveness Data Page 16 {16} PMA P180039: FDA Summary of Safety and Effectiveness Data Page 17 | Age Range | Gender | LIAISON XL MUREX | | | | | | --- | --- | --- | --- | --- | --- | --- | | | | + | | - | | Total | | | | n | % | n | % | | | 70-79 | F | 15 | 32.6% | 31 | 67.4% | 46 | | | M | 16 | 41.0% | 23 | 59.0% | 39 | | 80-89 | F | 8 | 57.1% | 6 | 42.9% | 14 | | | M | 2 | 28.6% | 5 | 71.4% | 7 | | 90-98 | F | 4 | 100.0% | 0 | 0% | 4 | | | M | 0 | 0% | 0 | 0% | 0 | | Unk | F | 1 | 100.0% | 0 | 0% | 1 | | | M | 1 | 100.0% | 0 | 0% | 1 | | Total | | 1306 | 48.8% | 1370 | 51.2% | 2676 | ## Hepatitis B Status Classification Hepatitis B Status Classification was based on testing all the samples with FDA approved HBV assays for HBsAg, HBeAg, Anti-HBc, Anti-HBc IgM, Anti-HBe and Anti-HBs. HBV classification for the prospective and retrospective specimens is presented below. Table 8: Hepatitis B Status Classification | HBV Classification | HBsAg | HBeAg | Total Anti-HBc | Anti-HBc IgM | Anti-HBe | Anti-HBs | Prospective (n) | Retrospective (n) | | --- | --- | --- | --- | --- | --- | --- | --- | --- | | Acute | R | NR | NR | NR | NR | NR | 12 | 97 | | Acute | R | R | NR | NR | NR | NR | | Acute | R | R | R | R | NR | NR | | Acute | R | R | R | R | R | NR | | Acute | R | R | R | R | EQV | NR | | Acute | R | NR | R | EQV | R | NR | | Acute | R | NR | R | R | EQV | NR | | Acute | R | R | R | R | NR | NR | | Acute | R | R | R | R | R | R | | Acute | R | R | R | R | R | R | | Acute | R | R | R | R | R | R | | Rate Acute | R | NR | R | R | R | NR | 2 | 32 | | Late Acute | R | NR | R | R | R | R | | Late Acute | R | NR | R | R | R | R | 2 | 32 | | Chronic | R | NR | NR | NR | R | NR | 76 | 68 | {17} | HBV Classification | HBsAg | HBeAg | Total Anti-HBc | Anti-HBc IgM | Anti-HBe | Anti-HBs | Prospective (n) | Retrospective (n) | | --- | --- | --- | --- | --- | --- | --- | --- | --- | | Chronic | R | NR | R | NR | NR | R | | | | Chronic | R | R | R | NR | NR | R | | | | Chronic | R | R | R | NR | NR | NR | | | | Chronic | R | EQV | R | NR | NR | NR | | | | Chronic | R | NR | R | NR | R | NR | | | | Chronic | R | NR | R | NR | NR | NR | | | | Chronic | R | NR | R | NR | R | R | | | | Chronic | R | EQV | R | NR | NR | NR | | | | Early Recovery | NR | NR | R | R | R | NR | 48 | 9 | | Early Recovery | NR | NR | R | EQV | R | R | | | | Early Recovery | NR | NR | R | R | NR | NR | | | | Early Recovery | NR | NR | R | NR | R | NR | | | | Early Recovery | NR | NR | R | NR | NR | NR | | | | Early Recovery | NR | NR | R | R | NR | R | | | | Early Recovery | NR | NR | R | R | R | R | | | | Recovery | NR | NR | R | NR | R | R | 131 | 36 | | Recovery | NR | NR | NR | NR | R | R | | | | Recovery | NR | NR | R | NR | EQV | R | | | | Immune Due to Natural Infection | NR | NR | R | NR | NR | R | 104 | 3 | | Immune Due to Natural Infection | NR | NR | R | NR | NR | EQV | | | | HBV Vaccine Response | NR | NR | NR | NR | NR | R | 1144 | 8 | | HBV Vaccine Response | NR | NR | NR | NR | NR | EQV | | | | Not Previously Infected | NR | NR | NR | NR | NR | NR | 1302 | 1 | PMA P180039: FDA Summary of Safety and Effectiveness Data {18} | HBV Classification | HBsAg | HBeAg | Total Anti-HBc | Anti-HBc IgM | Anti-HBe | Anti-HBs | Prospective (n) | Retrospective (n) | | --- | --- | --- | --- | --- | --- | --- | --- | --- | | Not Interpretable | NR | NR | NR | NR | R | NR | 7 | 2 | | Not Interpretable | NR | NR | NR | R | NR | NR | | | | Not Interpretable | NR | R | NR | NR | NR | NR | | | | Not Interpretable | NR | R | NR | NR | NR | R | | | | Not Interpretable | NR | R | R | R | NR | EQV | | | | Not Interpretable | NR | R | R | R | NR | R | | | | Not Interpretable | R | NR | NR | NR | NR | R | | | | Total | | | | | | | 2826 | 256 | ## Clinical Agreement Study Analysis Comparison results of the LIAISON XL MUREX Anti-HBs to the reference anti-HBs assay are presented with Negative and Positive percent (%) agreement and 95% confidence intervals for combined prospective and retrospective specimens for each of the HBV Classification categories. In addition, Pediatric Cumulative (prospective and retrospective) Clinical Agreement results are presented below. Table 9: Cumulative Clinical Agreement (Combined Prospective &amp; Retrospective) | HBV Classification | Reference Anti-HBs assay | | | | | | Total | | --- | --- | --- | --- | --- | --- | --- | --- | | | Reactive | | Eqv | | Non reactive | | | | | LIAISON XL MUREX Anti-HBs | | LIAISON XL MUREX Anti-HBs | | LIAISON XL MUREX Anti-HBs | | | | | Positive | Negative | Positive | Negative | Positive | Negative | | | Acute | 2 | 2 | 0 | 1 | 0 | 104 | 109 | | Late Acute | 1 | 1 | 0 | 0 | 0 | 32 | 34 | | Chronic | 3 | 1 | 0 | 0 | 1 | 139 | 144 | | Early Recovery | 8 | 0 | 0 | 0 | 9 | 40 | 57 | | Recovery | 163 | 4 | 0 | 0 | 0 | 0 | 167 | | Immune Due to Natural Infection | 103 | 0 | 3 | 1 | 0 | 0 | 107 | PMA P180039: FDA Summary of Safety and Effectiveness Data {19} | HBV Classification | Reference Anti-HBs assay | | | | | | Total | | --- | --- | --- | --- | --- | --- | --- | --- | | | Reactive | | Eqv | | Non reactive | | | | | LIAISON XL MUREX Anti-HBs | | LIAISON XL MUREX Anti-HBs | | LIAISON XL MUREX Anti-HBs | | | | | Positive | Negative | Positive | Negative | Positive | Negative | | | HBV Vaccine Response | 1106 | 14 | 16 | 16 | 0 | 0 | 1152 | | Not Previously Infected | 0 | 0 | 0 | 0 | 29 | 1274 | 1303 | | Not Interpretable | 3 | 0 | 0 | 1 | 0 | 5 | 9 | | Total | 1389 | 22 | 19 | 19 | 39 | 1594 | 3082 | Table 10: Cumulative Clinical Agreement (Combined Prospective &amp; Retrospective) | HBV Classification | Positive Percent Agreement (PPA) | Negative Percent Agreement (NPA) | | --- | --- | --- | | Acute | 2/5 (40.0%) 95% CI: 11.8% to 76.9% | 104/104 (100.0%) 95% CI: 96.4% to 100.0% | | Late Acute | 1/2 (50.0%) 95% CI: 9.5% to 90.5% | 32/32 (100.0%) 95% CI: 89.3% to 100.0% | | Chronic | 3/4 (75.0%) 95% CI: 30.1% to 95.4% | 139/140 (99.3%) 95% CI: 96.1% to 99.9% | | Early Recovery | 8/8 (100.0%) 95% CI: 67.6% to 100.0% | 40/49 (81.6%) 95% CI: 68.6% to 90.0% | | Recovery | 163/167 (97.6%) 95% CI: 94.0% to 99.1% | N/A | | Immune Due to Natural Infection | 103/104 (99.0%) 95% CI: 94.8% to 99.8% | 0/3 (0.0%) 95% CI: 0.0% to 56.2% | | HBV Vaccine Response | 1106/1136 (97.4%) 95% CI: 96.3% to 98.1% | 0/16 (0.0%) 95% CI: 0.0% to 19.4% | | Not Previously Infected | N/A | 1274/1303 (97.8%) 95% CI: 96.8% to 98.4% | | Not Interpretable | 3/4 (75.0%) 95% CI: 30.1% to 95.4% | 5/5 (100.0%) 95% CI: 56.6% to 100.0% | | Total | 1389/1430 (97.1%) 95% CI: 96.1% to 97.9% | 1594/1652 (96.5%) 95% CI: 95.5% to 97.3% | ## Clinical Endpoints With regard to safety, as an *in vitro* diagnostic test, the LIAISON XL MUREX Anti-HBs test involves taking a sample of plasma or serum from a patient. The test, therefore, presents PMA P180039: FDA Summary of Safety and Effectiveness Data {20} no more safety hazard to an individual being tested than other tests where blood samples are drawn. Safety issues regarding false positive and negative test results are discussed in section VIII. With regard to effectiveness, the clinical performance of the LIAISON XL MUREX Anti-HBs was evaluated versus a FDA approved anti-HBs test for patients at risk for infection with hepatitis B and for patients with signs and symptoms of hepatitis. With regard to success/failure criteria, the assay performed well with a positive percent agreement (PPA) of 97.1% a negative percent agreement (NPA) of 96.5% among subjects in various stages of HBV infection, a PPA of 97.4% in HBV-vaccinated subjects, a PPA of 99.0% in subjects immune due to natural infection, and an NPA of 97.8% among subjects not previously infected with HBV. ## B. Accountability of PMA Cohort The clinical agreement study involved the testing of 3,082 samples on six (6) FDA approved reference assays, each detecting a unique serological marker (HBsAg, HBeAg, Anti-HBs, Anti-HBc, Anti-HBc IgM, and Anti-HBe in order determine the HBV classification for each of the samples tested. The samples were collected from 6 different countries: Russia, Colombia, Cameroon, Ghana, Nigeria, and the United States. The U.S. samples were from multiple states including Ohio, Pennsylvania, Indiana, Florida, California, Texas, New Jersey, Tennessee, Massachusetts, and Puerto Rico. ## C. Study Population Demographics and Baseline Parameters The demographics of the study population are typical for an anti-HBs detection study performed in the US. The prospective (unselected) subjects were defined as follows: - Pediatric and adult male (38.2%), female (61.6%) and unknown gender (0.2%) subjects at risk for hepatitis due to medical conditions (dialysis, transplantation), occupation, lifestyle, behavior or a known exposure event. - Subjects showing signs or symptoms and individuals living in an area with a higher probability of HBV infection. - The demographic breakdown of the prospective population was as follows: American Indian/Alaskan Native (0.1%), Asian (0.8%), Black/African American (31.2%), Caucasian (62.5%), Other (5.2%), and Unknown (0.2%) with an age range of 2 - 98 years of age. The retrospective (selected/archived) samples were from male (69.5%), female (21.9%), and unknown gender (8.6%) subjects diagnosed with Acute and/or Chronic Hepatitis having an age range of 17 - 67 years of age from the following ethnicities: Asian (1.6%), PMA P180039: FDA Summary of Safety and Effectiveness Data Page 21 {21} Black/African American (23.8%), Caucasian (73%), other (1.2%) and 0.4% Unknown. The table below shows the demographic distribution of the cohort. Table11: Prospective and Retrospective Demographic Summary | | Adult | | | | Pediatric (2-21) | | | | Unknown Age | | | | | --- | --- | --- | --- | --- | --- | --- | --- | --- | --- | --- | --- | --- | | | Prospective | | Retrospective | | Prospective | | Retrospective | | Prospective | | Retrospective | | | Race | n | % | n | % | n | % | n | % | n | % | n | % | | American Indian/Alaskan Native | 2 | 0.1% | 0 | 0.0% | 0 | 0.0% | 0 | 0.0% | 0 | 0.0% | 0 | 0.0% | | Asian | 21 | 0.8% | 4 | 1.9% | 3 | 1.9% | 0 | 0.0% | 0 | 0.0% | 0 | 0.0% | | Black/African American | 832 | 31.2% | 57 | 27.7% | 64 | 39.8% | 4 | 13.8% | 0 | 0.0% | 0 | 0.0% | | Native Hawaiian or Other Pacific Islander | 0 | 0.0% | 0 | 0.0% | 0 | 0.0% | 0 | 0.0% | 0 | 0.0% | 0 | 0.0% | | White | 1664 | 62.5% | 141 | 68.4% | 89 | 55.3% | 25 | 86.2% | 2 | 100.0% | 21 | 100.0% | | Unknown | 6 | 0.2% | 1 | 0.5% | 0 | 0.0% | 0 | 0.0% | 0 | 0.0% | 0 | 0.0% | | Other | 138 | 5.2% | 3 | 1.5% | 5 | 3.1% | 0 | 0.0% | 0 | 0.0% | 0 | 0.0% | | Total | 2663 | 100.0% | 206 | 100.0% | 161 | 100.0% | 29 | 100.0% | 2 | 100.0% | 21 | 100.0% | ## D. Safety and Effectiveness Results ### 1. Safety Results With regard to safety, as an in vitro diagnostic test, the LIAISON XL MUREX Anti-HBs test involves taking a sample of plasma or serum from a patient. The test, therefore, presents no more safety hazard to an individual being tested than other tests where blood samples are drawn. There were no adverse effects that occurred in the PMA clinical study. ### 2. Effectiveness Results The analysis of effectiveness was based on the 3,082 evaluable patients. Key effectiveness outcomes are presented in the tables below. PMA P180039: FDA Summary of Safety and Effectiveness Data {22} Table 12: Clinical Comparison for Prospectively Collected Samples | HBV Classification | Roche Anti-HBs | | | | | | Total | | --- | --- | --- | --- | --- | --- | --- | --- | | | + | | Eqv | | - | | | | | LIAISON XL MUREX Anti-HBs | | LIAISON XL MUREX Anti-HBs | | LIAISON XL MUREX Anti-HBs | | | | | + | - | + | - | + | - | | | Acute | 0 | 0 | 0 | 0 | 0 | 12 | 12 | | Late Acute | 0 | 0 | 0 | 0 | 0 | 2 | 2 | | Chronic | 3 | 1 | 0 | 0 | 1 | 71 | 76 | | Early Recovery | 5 | 0 | 0 | 0 | 8 | 35 | 48 | | Recovery | 127 | 4 | 0 | 0 | 0 | 0 | 131 | | Immune Due to Natural Infection | 100 | 0 | 3 | 1 | 0 | 0 | 104 | | HBV Vaccine Response | 1099 | 13 | 16 | 16 | 0 | 0 | 1144 | | Not Previously Infected | 0 | 0 | 0 | 0 | 29 | 1273 | 1302 | | Not Interpretable | 1 | 0 | 0 | 1 | 0 | 5 | 7 | | Total | 1335 | 18 | 19 | 18 | 38 | 1398 | 2826 | Table 13: Percent Agreement for Prospectively Collected Samples | HBV Classification | Positive Percent Agreement (PPA) | Negative Percent Agreement (NPA) | | --- | --- | --- | | Acute | N/A | 12/12 (100.0%) 95% CI: 75.7% to 100.0% | | Late Acute | N/A | 2/2 (100.0%) 95% CI: 34.2% to 100.0% | | Chronic | 3/4 (75.0%) 95% CI: 30.1% to 95.4% | 71/72 (98.6%) 95% CI: 92.5% to 99.8% | | Early Recovery | 5/5 (100.0%) 95% CI: 56.6% to 100.0% | 35/43 (81.4%) 95% CI: 67.4% to 90.3% | | Recovery | 127/131 (96.9%) 95% CI: 92.4% to 98.8% | N/A | | Immune Due to Natural Infection | 100/101 (99.0%) 95% CI: 94.6% to 99.8% | 0/3 (0.0%) 95% CI: 0.0% to 56.2% | | HBV Vaccine Response | 1099/1128 (97.4%) 95% CI: 96.3% to 98.1% | 0/16 (0.0%) 95% CI: 0.0% to 19.4% | | Not Previously Infected | N/A | 1273/1302 (97.8%) 95% CI: 96.8% to 98.4% | | Not Interpretable | 1/2 (50.0%) 95% CI: 9.5% to 90.5% | 5/5 (100.0%) 95% CI: 56.6% to 100.0% | | Total | 1335/1371 (97.4%) 95% CI: 96.4% to 98.1% | 1398/1455 (96.1%) 95% CI: 95.0% to 97.0% | PMA P180039: FDA Summary of Safety and Effectiveness Data {23} Table 14: Clinical Comparison for Retrospectively Collected Samples | HBV Classification | Roche Anti-HBs | | | | | | Total | | --- | --- | --- | --- | --- | --- | --- | --- | | | + | | Eqv | | - | | | | | LIAISON XL MUREX Anti-HBs | | LIAISON XL MUREX Anti-HBs | | LIAISON XL MUREX Anti-HBs | | | | | + | - | + | - | + | - | | | Acute | 2 | 2 | 0 | 1 | 0 | 92 | 97 | | Late Acute | 1 | 1 | 0 | 0 | 0 | 30 | 32 | | Chronic | 0 | 0 | 0 | 0 | 0 | 68 | 68 | | Early Recovery | 3 | 0 | 0 | 0 | 1 | 5 | 9 | | Recovery | 36 | 0 | 0 | 0 | 0 | 0 | 36 | | Immune Due to Natural Infection | 3 | 0 | 0 | 0 | 0 | 0 | 3 | | HBV Vaccine Response | 7 | 1 | 0 | 0 | 0 | 0 | 8 | | Not Previously Infected | 0 | 0 | 0 | 0 | 0 | 1 | 1 | | Not Interpretable | 2 | 0 | 0 | 0 | 0 | 0 | 2 | | Total | 54 | 4 | 0 | 1 | 1 | 196 | 256 | Table 15: Percent Agreement for Retrospectively Collected Samples | HBV Classification | Positive Percent Agreement (PPA) | Negative Percent Agreement (NPA) | | --- | --- | --- | | Acute | 2/5 (40.0%) 95% CI: 11.8% to 76.9% | 92/92 (100.0%) 95% CI: 96% to 100.0% | | Late Acute | 1/2 (50.0%) 95% CI: 9.5% to 90.5% | 30/30 (100.0%) 95% CI: 88.6% to 100.0% | | Chronic | N/A | 68/68 (100.0%) 95% CI: 94.7% to 100.0% | | Early Recovery | 3/3 (100.0%) 95% CI: 43.8% to 100.0% | 5/6 (83.3%) 95% CI: 43.6% to 97.0% | | Recovery | 36/36 (100.0%) 95% CI: 90.4% to 100.0% | N/A | | Immune Due to Natural Infection | 3/3 (100.0%) 95% CI: 43.8% to 100.0% | N/A | | HBV Vaccine Response | 7/8 (87.5%) 95% CI: 52.9% to 97.8% | N/A | | Not Previously Infected | N/A | 1/1 (100.0%) 95% CI: 20.7% to 100.0% | | Not Interpretable | 2/2 (100.0%) 95% CI: 34.2% to 100.0% | N/A | | Total | 54/59 (91.5%) 95% CI: 81.6% to 96.8% | 196/197 (99.5%) 95% CI: 97.8% to 99.9% | PMA P180039: FDA Summary of Safety and Effectiveness Data Page 24 {24} Table 16: Pediatric- Percent Agreement for Prospectively Collected Samples | HBV Classification | Prospective Age in Years | Positive Percent Agreement (PPA) | Negative Percent Agreement (NPA) | | --- | --- | --- | --- | | Acute | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | NA | NA | | Late Acute | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | NA | NA | | Chronic | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | NA | 4/5 (80.0%) 37.6%-96.4% | | Early Recovery | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | NA | NA | | Recovery | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | 4/5 (80.0%) 37.6%-96.4% | NA | | Immune Due to Natural Infection | 2-12 | NA | NA | | | 13-18 | 2/2 (100.0%) 34.2%-100.0% | NA | | | 19-21 | 1/1 (100.0%) 20.7%-100.0% | NA | | HBV Vaccine Response | 2-12 | 16/16 (100.0%) 80.6%-100.0% | 0/1 (0.0%) 0.0%-79.3% | | | 13-18 | 14/16 (87.5%) 64.0%-96.5% | NA | | | 19-21 | 26/27 (96.3%) 81.7%-99.3% | 0/2 (0.0%) 0.0%-65.8% | | Not Previously Infected | 2-12 | NA | 12/12 (100.0%) 75.7%-100.0% | | | 13-18 | NA | 11/13 (84.6%) 57.8%-95.7% | | | 19-21 | NA | 55/59 (93.2%) 83.8%-97.3% | | Not Interpretable | 2-12 | NA | 1/1 (100.0%) 20.7%-100.0% | | | 13-18 | NA | NA | | | 19-21 | NA | 1/1 (100.0%) 20.7%-100.0% | PMA P180039: FDA Summary of Safety and Effectiveness Data {25} Table 17: Pediatric- Percent Agreement for Retrospectively Collected Samples | HBV Classification | Retrospective Age in Years | Positive Percent Agreement (PPA) | Negative Percent Agreement (NPA) | | --- | --- | --- | --- | | Acute | 2-12 | NA | NA | | | 13-18 | NA | 6/6 (100.0%) 61.0%-100.0% | | | 19-21 | NA | 14/14 (100.0%) 78.5%-100.0% | | Late Acute | 2-12 | NA | NA | | | 13-18 | NA | 3/3 (100.0%) 43.8%-100.0% | | | 19-21 | NA | 4/4 (100.0%) 51.0%-100.0% | | Chronic | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | NA | 2/2 (100.0%) 34.2%-100.0% | | Early Recovery | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | NA | 1/1 (100.0%) 20.7%-100.0% | | Recovery | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | NA | NA | | Immune Due to Natural Infection | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | NA | NA | | HBV Vaccine Response | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | 1/1 (100.0%) 20.7%-100.0% | NA | | Not Previously Infected | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | NA | NA | | Not Interpretable | 2-12 | NA | NA | | | 13-18 | NA | NA | | | 19-21 | NA | NA | PMA P180039: FDA Summary of Safety and Effectiveness Data Page 26 {26} PMA P180039: FDA Summary of Safety and Effectiveness Data Page 27 3. **Subgroup Analyses** The study design enabled an assessment of assay performance by subgroup as depicted in tables above which show subjects stratified by stage of HBV infection and HBV vaccine response. 4. **Pediatric Extrapolation** In this premarket application, existing clinical data from adult subjects was not leveraged to support approval of a pediatric patient population. Samples from pediatric patients were tested in the clinical study in order to support a pediatric claim. E. **Financial Disclosure** The Financial Disclosure by Clinical Investigators regulation (21 CFR 54) requires applicants who submit a marketing application to include certain information concerning the compensation to, and financial interests and arrangement of, any clinical investigator conducting clinical studies covered by the regulation. The pivotal clinical study included 3 investigators. None of the clinical investigators had disclosable financial interests/arrangements as defined in sections 54.2(a), (b), (c), and (f). The information provided does not raise any questions about the reliability of the data. XI. **PANEL MEETING RECOMMENDATION AND FDA’S POST-PANEL ACTION** In accordance with the provisions of section 515(c)(3) of the act as amended by the Safe Medical Devices Act of 1990, this PMA was not referred to the Microbiology Panel, an FDA advisory committee, for review and recommendation because the information in the PMA substantially duplicates information previously reviewed by this panel. XII. **CONCLUSIONS DRAWN FROM PRECLINICAL AND CLINICAL STUDIES** A. **Effectiveness Conclusions** The effectiveness of the LIAISON XL MUREX Anti-HBs test for the qualitative and quantitative determination of antibodies to hepatitis-B surface antigen in human serum and plasma (lithium and sodium heparin and K2 EDTA) samples including separator tubes, on the LIAISON XL Analyzer has been demonstrated in the following patient populations: adults and pediatric patients (2 – 21 years). The results of this test may be used as an aid in the diagnosis of hepatitis B virus (HBV) infection in patients with symptoms of hepatitis or who may be at risk for hepatitis B infection. The results of this test may be used as an aid in the determination of susceptibility to HBV infection in individuals prior to or following HBV vaccination or where vaccination status is unknown. The positive agreement of the assay is 97.1% with a two-sided 95% {27} confidence interval (CI) of 96.1% - 97.1% and the negative percent agreement is 96.5% with a two-sided 95% CI of 95.5 - 97.3%. ## B. Safety Conclusions The risks of the device are based on nonclinical laboratory studies as well as data collected in a clinical study conducted to support PMA approval as described above. Based on the results of these studies the LIAISON XL MUREX Anti-HBs assay when used according to the manufacturer's instructions can aid the physician in the diagnosis of HBV infection and in the determination of susceptibility to HBV infection. The positive agreement of the assay is 97.1% with a two-sided 95% confidence interval (CI) of 96.1% - 97.1% and the negative percent agreement is 96.5% with a two-sided 95% CI of 95.5 - 97.3%. ## C. Benefit-Risk Determination The probable benefits of the device are also based on data collected in a clinical study conducted to support PMA approval as described above. The benefits of the assay are the determination of susceptibility to hepatitis B virus infection before or following vaccination, or as part of a hepatitis B panel, the appropriate diagnosis and treatment of hepatitis B infection. Treatment or vaccination for appropriate patients can mitigate the sequelae of hepatitis B infection and may result in improved morbidity and mortality in these patients. Known sequelae of hepatitis B infection include continued symptoms, increases in all-cause mortality, liver disease-related complications and death, hepato-cellular carcinoma rates, and need for liver transplantation. Additionally, diagnosis and appropriate treatment or appropriate vaccination for hepatitis B infection can potentially decrease transmission and disease burden in the general population and particularly in populations at high risk for hepatitis B infection. While the performance of the LIAISON XL MUREX Anti-HBs assay in the clinical study suggests that patients will benefit from the assay, low prevalence of certain HBV classifications (namely acute infection, chronic infection, and early recovery) is a source of potential uncertainty when analyzing the prospective and retrospective samples. The wide confidence intervals for those subgroups is expected due to the biology of hepatitis B infection and is acceptable. The probable risks of the device are also based on data collected in a clinical study conducted to support PMA approval as described above. Risks of false positive results when the device is used as an aid in the diagnosis of hepatitis B virus (HBV) infection in patients with symptoms of hepatitis or who may be at risk for HBV infection include improper patient management, including treatment for hepatitis B with antiviral medication. Antiviral medication has risks including toxicity and more rarely allergic reactions. Over time, viral resistance in patients who are coinfected PMA P180039: FDA Summary of Safety and Effectiveness Data Page 28 {28} but undiagnosed with other viruses that are treated with the same antiviral medication, such as HIV, can lead to viral resistance, however the chance of an undiagnosed coinfection in a patient treated for hepatitis B is unlikely. Risks of false positive results when the device is used as an aid in the determination of susceptibility to HBV infection in individuals prior to or following HBV vaccination or where vaccination status is unknown includes leading a provider to falsely believe that a patient has been vaccinated in the past and/or has current immunity when the patient, in fact, does not. This could lead to a patient inappropriately missing a vaccination. Risks of false negative results when the device is used as an aid in the diagnosis of HBV infection in patients with symptoms of hepatitis or who may be at risk for HBV infection include potentially missing and undertreating a patient who has hepatitis B infection. Missing and under-treating a patient with hepatitis B infection whose clinical picture warrants antiviral treatment could result in the known sequelae of HBV infection and may result in high morbidity and mortality in these patients. Additionally, missing a diagnosis of hepatitis B infection will not allow for clinicians to potentially decrease transmission and disease burden in the general population, particularly in populations at high risk for hepatitis B infection. Risks of false negative results when the device is used as an aid in the determination of susceptibility to HBV infection in individuals prior to or following HBV vaccination or where vaccination status is unknown include unnecessary repeated vaccination for hepatitis B. Although vaccination has risks such as local reactions, administrations of extra doses of single-antigen hepatitis B vaccine is not inherently harmful. In fact, it is common practice to administer higher dose vaccinations in an accelerated schedule for patients undergoing organ transplantation, for example. 1. Patient Perspectives This submission did not include specific information on patient perspectives for this device. In conclusion, given the available information above, the data support the claimed intended use, the probable benefits outweigh the probable risks. D. Overall Conclusions The data in this application support the reasonable assurance of safety and effectiveness of this device when used in accordance with the indications for use. The probable clinical benefits outweigh the potential risks for the proposed assay considering the performance of the device in the clinical trial and the low risk and associated risk mitigations in clinical practice. The proposed assay labelling will facilitate accurate assay implementation and interpretation of results. The clinical performance observed in the prospective and retrospective clinical trial suggests that errors will be uncommon and that the assay may provide substantial benefits to PMA P180039: FDA Summary of Safety and Effectiveness Data Page 29 {29} patients as an accurate and sensitive aid in the diagnosis of HBV infection when used in conjunction with other laboratory results and clinical information or for the determination of susceptibility to HBV infection in individuals prior to or following HBV vaccination or where vaccination status is unknown. ## XIII. CDRH DECISION CDRH issued an approval order on February 21, 2020. The applicant’s manufacturing facilities have been inspected and found to be in compliance with the device Quality System (QS) regulation (21 CFR 820). ## XIV. APPROVAL SPECIFICATIONS Directions for use: See device labeling. Hazards to Health from Use of the Device: See Indications, Contraindications, Warnings, Precautions, and Adverse Events in the device labeling. Post-approval Requirements and Restrictions: See approval order. PMA P180039: FDA Summary of Safety and Effectiveness Data Page 30