ELECSYS T3

{0} AUG 15 1996 510(k) Summary K962508 ## Introduction According to the requirements of 21 CFR 807.92, the following information provides sufficient detail to understand the basis for a determination of substantial equivalence. ### 1) Submitter name, address, contact Boehringer Mannheim Corporation 9115 Hague Rd. Indianapolis, IN 46250 (317) 845-2000 Contact Person: LeeAnn Chambers Date Prepared: June 24, 1996 ### 2) Device name Proprietary name: Elecsys T3 Common name: Total triiodothyronine test system ### 3) Predicate device We claim substantial equivalence to the Enzymun-Test® T3. ### 4) Device Description The Elecsys® T3 employs a competitive test principle with polyclonal antibodies directed against T3 and with streptavidin microparticles and electrochemiluminescence detection. Total duration of assay: 18 minutes. - 1st Incubation: Sample (30 µl) and specific anti-T3 antibodies labeled with a ruthenium complex together with ANS to release T3 from serum. - 2nd Incubation: After the addition of streptavidin-coated microparticles and biotinylated T3, the still-free binding sites of the labeled antibody become occupied, with formation of an antibody-hapten complex. The entire complex is bound to the solid phase via interaction of biotin and streptavidin. Continued on next page {1} AUG 15 1996 510(k) Summary, Continued 4) Device Description (cont.) - The reaction mixture is aspirated into the measuring cell where the microparticles are magnetically captured onto the surface of the electrode. Unbound substances are then removed with ProCell. Application of a voltage to the electrode then induces chemiluminescent emission which is measured by a photomultiplier. - Results are determined via a calibration curve which is instrument-specifically generated by 2-point calibration and a master curve provided via the reagent bar code. 5) Intended use For the in vitro quantitative determination of total triiodothyronine (T3) in human serum and plasma. 5) Indications for use Triiodothyronine (T3) is the hormone principally responsible for the development of the effects of the thyroid hormones on the various target organs. T3 (3.5,3’ Triiodothyronine) is mainly formed extra-thyroidally, particularly in the liver, by enzymatic 5’-deiodination of T4. Accordingly, the T3 concentration in serum is more a reflection of the functional state of the peripheral tissue than the secretory performance of the thyroid gland. A reduction in the conversion of T4 to T3 results in a fall in the T3 concentration. It occurs under the influence of medications such as propanolol, glucocorticoids or amiodarone and in severe non-thyroidal general diseases - “non-thyroidal illness” (NTI) - and is referred to as the “low T3 syndrome.” Like T4, over 99% of T3 is bound to transport proteins, but its affinity to them is around 10-fold lower.¹⁻³,⁷ Continued on next page {2} 510(k) Summary, Continued 24 5) Indications for use The determination of T3 is utilized in the diagnosis of T3-hyperthyroidism, the detection of early stages of hyperthyroidism and for indicating a diagnosis of thyrotoxicosis factitia.4-6 References 1. Wheeler MH, Lazarus JH. Diseases of the Thyroid. Chapman and Hall Medical. London Glasgow Weinheim New York Tokyo Melbourne Madras 1994;107-115. 2. Pfannenstiel P, Saller B. Schilddrüsenkrankheiten Diagnose und Therapie. Berliner Medizinische Verlagsanstalt GmbH 1995; 2:30-32,60-62. 3. Fisher DA. Physiological variations in thyroid hormones physiological and pathophysiological considerations. Clinical Chemistry 1996;42:135-139. 4. Klee GG. Clinical usage recommendations and analytic performance goals for total and free triiodothyronine measurements. Clinical Chemistry 1996;42:155-159. 5. Surks MI, Chopra IJ, Mariash CN, Nicoloff JT, Solomon DH. American Thyroid Association guidelines for use of laboratory tests in thyroid disorders. JAMA 1990;63:1529-1532. 6. Becker DV, Bigos ST, Gaitan E, Morris JC, Rallison ML, Spencer CA, et at. Optimal use of blood tests for assessment of thyroid function (letter). JAMA 1993. 269:273. 7. Wild D. The Immunoassay Handbook. Stockton Press 1994; 338. 6) Comparison to predicate device The Boehringer Mannheim Elecsys T3 is substantially equivalent to other products in commercial distribution intended for similar use. Most notably it is substantially equivalent to the currently marketed Enzymun-Test® T3. Similarities: - Intended use: immunoassay for the in vitro quantitative determination of Total Triiodothyronine (T3) - Competitive test principle - Sample type: serum and plasma - Antibody: sheep anti-T3 polyclonal - Capture principle: streptavidin / biotin Continued on next page {3} 510(k) Summary, Continued 2004-2014 Guahrouer ## 6) Comparison to predicate device (cont.) ### Differences: | Feature | Elecsys T3 | Enzymun-Test T3 | | --- | --- | --- | | Reaction test principle | streptavidin microparticles and electrochemiluminescence technology | streptavidin-coated tubes and enzyme immunoassay technology | | Sample volume | 30 μl | 100 μl | | Instrument required | Elecsys 2010 | ES 300 | | Calibration | a two point calibration renewal is recommended every 7 days or 1 month if the same reagent lot is used and the reagent pack is consumed within 7 days | a full calibration curve run is recommended every 2 weeks | ### Performance Characteristics: | Feature | Elecsys T3 | | | | | Enzymun-Test® T3 | | | | --- | --- | --- | --- | --- | --- | --- | --- | --- | | Precision: | NCCLS (modified) (EP5-T2): | | | | | Modified NCCLS “Midi” (EP3-T) | | | | Sample | PC U1 | PC U2 | HS1 | HS2 | HS3 | 1 | 2 | 3 | | N | 60 | 60 | 60 | 60 | 60 | 118 | 120 | 117 | | Mean (nmol/l) | 2.12 | 6.31 | 1.22 | 2.87 | 5.09 | 0.95 | 2.56 | 4.26 | | wi/in run % CV | 4.1 | 3.5 | 3.6 | 4.2 | 5.3 | 2.9 | 1.6 | 1.7 | | total run % CV | 4.8 | 4.1 | 5.4 | 4.7 | 5.4 | 4.7 | 2.2 | 2.8 | | Sensitivity | Lower Detection Limit: | | | | | Lower Detection Limit: | | | | | 0.3 nmol/l | | | | | 0.46 nmol/l | | | | | 0.19 ng/ml | | | | | 0.3 ng/ml | | | | Assay range | 0.3 - 10.00 nmol/l | | | | | 0.46 - 9.22 nmol/l | | | | (LDL to high std.) | 0.19 - 6.51 ng/ml | | | | | 0.3 - 6.0 ng/ml | | | Continued on next page {4} 510(k) Summary, Continued Guérinier F. Substantial equivalence, (cont.) Performance Characteristics: | Method Comparison | vs. Enzymun-Test T3 (Cat. # 1360868) Least Squares: N = 300 y = -0.35 + 1.18x r = 0.957 Passing/Bablok N = 300 y = -0.56 + 1.26x r = 0.957 | vs. Enzymun-Test T3 (Cat. # 1135287) Least Squares: N = 55 y = 1.13x + 0.02 r = 0.994 | | --- | --- | --- | | Interfering substance: Hemoglobin Lipemia Bilirubin Biotin | No interference up to: 1 g/dl 1500 mg/dl 25 mg/dl 20 ng/ml | No interference up to: 1 g/dl 1250 mg/dl 65 mg/dl 50 ng/ml | | Specificity D-T3 L-T4 D-T4 L-rT3 L-T2 3,3',5-tri-iodothyroacetic acid 3,3',5,5'-tetra-iodothyroacetic acid | % cross reaction 98.9 0.115 0.115 0.007 0.998 106.4 0.007 | % cross reaction 100 0.16 0.07 0.04 1.0 7.5 0.01 | {5} DEPARTMENT OF HEALTH & HUMAN SERVICES Public Health Service Food and Drug Administration 2098 Gaither Road Rockville MD 20850 AUG 15 1996 LeeAnn Chambers, RAC Program Manager, Regulatory Affairs Boehringer Mannheim Corporation Quality System & Compliance 9115 Hague Road P.O. Box 50457 Indianapolis, Indiana 46250-0457 Re: K962508 Elecsys T3 Regulatory Class: II Product Code: CDP, JIS Dated: July 25, 1996 Received: July 26, 1996 Dear Ms. Chambers: We have reviewed your Section 510(k) notification of intent to market the device referenced above and we have determined the device is substantially equivalent (for the indications for use stated in the enclosure) to devices marketed in interstate commerce prior to May 28, 1976, the enactment date of the Medical Device Amendments or to devices that have been reclassified in accordance with the provisions of the Federal Food, Drug, and Cosmetic Act (Act). You may, therefore, market the device, subject to the general controls provisions of the Act. The general controls provisions of the Act include requirements for annual registration, listing of devices, good manufacturing practice, labeling, and prohibitions against misbranding and adulteration. If your device is classified (see above) into either class II (Special Controls) or class III (Premarket Approval), it may be subject to such additional controls. Existing major regulations affecting your device can be found in the Code of Federal Regulations, Title 21, Parts 800 to 895. A substantially equivalent determination assumes compliance with the Good Manufacturing Practice for Medical Devices: General (GMP) regulation (21 CFR Part 820) and that, through periodic GMP inspections, the Food and Drug Administration (FDA) will verify such assumptions. Failure to comply with the GMP regulation may result in regulatory action. In addition, FDA may publish further announcements concerning your device in the Federal Register. Please note: this response to your premarket notification submission does not affect any obligation you might have under sections 531 through 542 of the Act for devices under the Electronic Product Radiation Control provisions, or other Federal Laws or Regulations. {6} Page 2 Under the Clinical Laboratory Improvement Amendments of 1988 (CLIA-88), this device may require a CLIA complexity categorization. To determine if it does, you should contact the Centers for Disease Control and Prevention (CDC) at (770)488-7655. This letter will allow you to begin marketing your device as described in your 510(k) premarket notification. The FDA finding of substantial equivalence of your device to a legally marketed predicate device results in a classification for your device and thus, permits your device to proceed to the market. If you desire specific advice for your device on our labeling regulation (21 CFR Part 801 and additionally 809.10 for in vitro diagnostic devices), please contact the Office of Compliance at (301) 594-4588. Additionally, for questions on the promotion and advertising of your device, please contact the Office of Compliance at (301) 594-4639. Also, please note the regulation entitled, "Misbranding by reference to premarket notification" (21 CFR 807.97). Other general information on your responsibilities under the Act may be obtained from the Division of Small Manufacturers Assistance at its toll free number (800) 638-2041 or at (301) 443-6597. Sincerely yours, Steven I. Gutman, M.D., M.B.A. Director Division of Clinical Laboratory Devices Office of Device Evaluation Center for Devices and Radiological Health Enclosure {7} 510(k) Number (if known): K-962508 Device Name: Elecsys® T3 Indications for Use: Triiodothyronine (T3) is the hormone principally responsible for the development of the effects of the thyroid hormones on the various target organs. T3 (3,5,3’ Triiodothyronine) is mainly formed extra-thyroidally, particularly in the liver, by enzymatic 5’-deiodination of T4. Accordingly, the T3 concentration in serum is more a reflection of the functional state of the peripheral tissue than the secretory performance of the thyroid gland. A reduction in the conversion of T4 to T3 results in a fall in the T3 concentration. It occurs under the influence of medications such as propanolol, glucocorticoids or amiodarone and in severe non-thyroidal general diseases - “non-thyroidal illness” (NTI) - and is referred to as the “low T3 syndrome.” Like T4, over 99% of T3 is bound to transport proteins, but its affinity to them is around 10-fold lower.¹⁻³,⁷ The determination of T3 is utilized in the diagnosis of T3-hyperthyroidism, the detection of early stages of hyperthyroidism and for indicating a diagnosis of thyrotoxicosis factitia.⁴⁻⁶ ## References 1. Wheeler MH, Lazarus JH. Diseases of the Thyroid. Chapman and Hall Medical. London: Glasgow Weinheim New York Tokyo Melbourne Madras 1994;107-115. 2. Pfannenstiel P, Saller B. Schilddrüsenkrankheiten Diagnose und Therapie. Berliner Medizinische Verlagsanstalt GmbH 1995; 2:30-32,60-62. 3. Fisher DA. Physiological variations in thyroid hormones physiological and pathophysiological considerations. Clinical Chemistry 1996;42:135-139. Continued on next page (PLEASE DO NOT WRITE BELOW THIS LINE - CONTINUE ON ANOTHER PAGE IF NEEDED) Concurrence of CDRH, Office of Device Evaluation (ODE) (Division Sign-Off) Division of Clinical Laboratory Devices 510(k) Number 6962508 OR Over-The-Counter Use (Optional Format 1-2-96) Prescription Use ☑ (Per 21 CFR 801.109) 20