The LZI Oral Fluid Amphetamine Enzyme Immunoassay is intended for the qualitative and semi-quantitative determination of d-amphetamine in neat human oral fluid, collected into the LZI Oral Fluid Collector, at the cutoff value 50 ng/mL. The assay is designed for prescription use with a number of automated clinical chemistry analyzers.

The semi-quantitative mode is for purposes of (1) enabling laboratories to determine an appropriate dilution of the specimen for confirmation by a confirmatory method such as GCMS and LCMS or (2) permitting laboratories to establish quality control procedures.

The LZI Oral Fluid Amphetamine Calibrators are for use as calibrators in the qualitative and semi-quantitative calibration of the LZI Oral Fluid Amphetamine Enzyme Immunoassay at the cutoff value 50 ng/mL.

The LZI Oral Fluid Amphetamine Controls are for use as assayed quality control materials to monitor the precision of the LZI Oral Fluid Amphetamine Enzyme Immunoassay at the cutoff value of 50 ng/mL.

The assay provides only a preliminary analytical result. A more specific alternative chemical method must be used in order to obtain a confirmed analytical result. Gas or liguid chromatography/mass spectrometry (GC/MS or LC/MS) is the preferred confirmatory method). Clinical consideration and professional judgment should be exercised with any drug of abuse test result, particularly when the preliminary test result is positive.

Device Description

The LZI Oral Fluid Amphetamine assay is a homogeneous enzyme immunoassay with ready-touse liquid reagent. The assay is based on competition between drug in the sample and drug labeled with the enzyme glucose-6-phosphate dehydrogenase (G6PDH) for a fixed amount of antibody in the reagent. Enzyme activity decreases upon binding to the antibody, and the drug concentration in the sample is measured in terms of enzyme activity. In the absence of drug in the sample, amphetamine-labeled G6PDH conjugate is bound to antibody, and the enzyme activity is inhibited. On the other hand, when free drug is present in the sample, antibody would bind to free drug, the unbound amphetamine-labeled G6PDH then exhibits its maximal enzyme activity. Active enzyme converts nicotinamide adenine dinucleotide (NAD) to NADH, resulting in an absorbance change that can be measured spectrophotometrically at 340 nm.

The LZI Oral Fluid Amphetamine Enzyme Immunoassay is a kit comprised of two reagents, an R1 and R2 which are bottled separately but sold together within the kit.

The R solution contains mouse monoclonal anti-amphetamine antibody, glucose-6-phosphate (G6P) nicotinamide adenine dinucleotide (NAD), stabilizers, and sodium azide (0.09%) as a preservative. The R2 solution contains glucose-6-phosphate dehydrogenase (G6PDH) labeled with amphetamine in buffer with sodium azide (0.09%) as preservative.

The LZI Oral Fluid Amphetamine Enzyme Immunoassay calibrators and controls designated for use at the 50 ng/mL cutoffs contain 0, 25, 37.5, 50, 62.5, 100, and 140 ng/mL of d-amphetamine in human oral fluid with sodium azide (0.09%) as preservative. These five calibrators and two controls are sold as individual bottles.

The LZI Oral Fluid Collector is a 50 mL polypropylene collection tube. It is a non-sterile centrifuge tube with a screw-on cap and printed graduations (United Lab Plastics, Catalog#UP2262).

AI/ML Overview

Here's a breakdown of the acceptance criteria and study information for the LZI Oral Fluid Amphetamine Enzyme Immunoassay, based on the provided 510(k) summary:

1. Table of Acceptance Criteria and Reported Device Performance

The acceptance criteria for this device are implied through the comparison to the predicate device and the presented performance data, particularly in the context of precision and method agreement. Explicit numerical "acceptance criteria" are not stated as clear, pre-defined thresholds in the provided summary, but rather performance results are reported for evaluation against accepted scientific principles for such assays.

Here's an interpretation based on the provided data:

Performance Metric	Acceptance Criteria (Implied/Expected)	Reported Device Performance (LZI Oral Fluid Amphetamine Enzyme Immunoassay)
Qualitative Detection (Precision)	Accurate classification of samples below cutoff as negative and above cutoff as positive (with expected variability at cutoff).
- Negative Samples (< 50 ng/mL)	100% Negative	100% Negative (for 0, 12.5, 25, 37.5 ng/mL - 88 determinations each)
- Positive Samples (> 50 ng/mL)	100% Positive	100% Positive (for 62.5, 75, 87.5, 100 ng/mL - 88 determinations each)
- Around Cutoff (50 ng/mL)	Expected variability in classification (some positive, some negative)	46 Positive / 42 Negative (out of 88 total determinations)
Semi-Quantitative Detection (Precision)	Similar to qualitative, with expected variability around the cutoff.
- Negative Samples (< 50 ng/mL)	100% Negative	100% Negative (for 0, 12.5, 25, 37.5 ng/mL - 88 determinations each)
- Positive Samples (> 50 ng/mL)	100% Positive	100% Positive (for 62.5, 75, 87.5, 100 ng/mL - 88 determinations each)
- Around Cutoff (50 ng/mL)	Expected variability in classification	36 Positive / 52 Negative (out of 88 total determinations)
Method Comparison (Clinical Samples)	High agreement with a confirmed analytical method (e.g., GC/MS or LC/MS).	100.0% agreement with negative samples; 97.7% agreement with positive samples
Linearity	Strong linear correlation across the analytical range.	R² = 0.9945 (y = 1.0555x - 0.7832) for range 0-140 ng/mL
Interference/Specificity	No significant undesired cross-reactivity or endogenous substance interference.	Reported as "No significant undesired cross reactants or endogenous substance interference was observed."
Stability (Shipping/Recovery)	No significant degradation of samples.	No significant sample degradation up to 72 hours.
Stability (Sample Storage)	No significant degradation of samples.	No significant sample degradation up to 13 days (2-8°C). Accelerated data supports 18 months at -20°C.
Stability (Open Vial Calibrator/Control)	Minimal degradation.	Minimal degradation for 17 months (568 days) at 2-8°C, RT, and 30°C.
Stability (Closed Reagent Shelf-life)	Minimal degradation.	Minimal degradation for 17 months (568 days) at 2-8°C.

2. Sample Size and Data Provenance for Test Set (Clinical Samples)

Sample Size: A total of eighty-five (85) clinical unaltered samples were used for the method comparison study.
Data Provenance: The document does not explicitly state the country of origin. It indicates they were "clinical unaltered samples," suggesting a prospective or retrospective collection from a clinical setting, but further details are not provided. Given the US FDA submission, it's highly probable the data was generated or collected in the US or under US regulatory standards.

3. Number of Experts and Qualifications for Ground Truth (Test Set)

The document does not mention the use of human experts to establish ground truth for the test set.
Instead, the ground truth for the clinical samples used in the "Method Comparison" was established by confirmatory analytical methods such as Gas Chromatography/Mass Spectrometry (GC/MS) or Liquid Chromatography/Mass Spectrometry (LC/MS). These are considered highly accurate and specific methods in toxicology testing.

4. Adjudication Method for the Test Set

None in the context of expert adjudication. The ground truth was established by independent, highly specific analytical methods (GC/MS or LC/MS), which are the gold standard for confirming drug presence. There was no need for expert consensus or adjudication in this type of analytical validation.

5. Multi-Reader Multi-Case (MRMC) Comparative Effectiveness Study

No, a MRMC comparative effectiveness study was not done. This device is an in-vitro diagnostic (IVD) enzyme immunoassay. Such assays are designed to produce a direct analytical result (positive/negative based on a cutoff, or semi-quantitative value) rather than interpreted by multiple human readers in the way, for example, a medical imaging AI would be. Therefore, the concept of "human readers improve with AI vs without AI assistance" does not apply to this type of device.

6. Standalone (Algorithm Only) Performance

Yes, a standalone performance study was done. The entire performance characterization section (Precision, Linearity, Method Comparison, Interference, Stability) describes the performance of the LZI Oral Fluid Amphetamine Enzyme Immunoassay as an analytical device, operating independently to produce results. There is no human-in-the-loop component for the initial diagnostic output of this specific immunoassay. It reports a direct result based on its enzymatic reaction and spectrophotometric measurement on an automated analyzer.

7. Type of Ground Truth Used

Confirmatory Analytical Methods: The ground truth for the clinical samples tested was established by Gas Chromatography/Mass Spectrometry (GC/MS) or Liquid Chromatography/Mass Spectrometry (LC/MS). These are the accepted gold standard methods for definitive drug confirmation in toxicology.

8. Sample Size for the Training Set

The document does not specify a separate "training set" or its size in the context of a machine learning algorithm. This device is an enzyme immunoassay, which is a biochemical reaction-based test, not a machine learning or AI-driven diagnostic.
The "training" of such a system typically refers to the calibration process. The immunoassay calibrators contain d-amphetamine at 0, 25, 37.5, 50, 62.5, 100, and 140 ng/mL. These are used to establish the standard curve for the assay on the automated analyzer.

9. How the Ground Truth for the Training Set was Established

As this is not a machine learning/AI device, there isn't a traditional "training set" with independent ground truth.
The "ground truth" for the calibrators (which are analogous to what might be used to define assay response) is established by their precisely manufactured and quantified d-amphetamine concentrations (e.g., 0 ng/mL, 25 ng/mL, 50 ng/mL, etc.) in human oral fluid matrix. These concentrations are analytically verified during the manufacturing process of the calibrators.

Summary

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Kj31653

510(k) Summary of Safety and Effectiveness

FEB - 4 2014

This summary of 510(k) safety and effectiveness information is being submitted in accordance with the requirements of SMDA 1990 and 21 CFR 807.92.

Preparation Date

January 30, 2014

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.

Submitter name, Address, and Contact

Lin-Zhi International, Inc. 670 Almanor Avenue Sunnyvale, CA 94085 Phone: (408) 732-3856 Fax: (408) 732-3849 e-mail: bclin@lin-zhi.com

Contact:	Bernice Lin, Ph.D.
	VP Operations

Device Name and Classification

Classification Name:	Enzyme Immunoassay, Oral Fluid AmphetamineClass II, DKZ (91 Toxicology),21 CFR 862.3100
	Drug Specific Calibrators,Class II, DLJ (91 Toxicology),21 CFR 862.3200
	Drug Specific Controls,Class I, LAS (91 Toxicology),21 CFR 862.3280
Common Name:Proprietary Name:	Homogeneous Oral Fluid Amphetamine Enzyme ImmunoassayLZI Oral Fluid Amphetamine Enzyme Immunoassay,LZI Oral Fluid Amphetamine CalibratorsLZI Oral Fluid Amphetamine Controls

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Legally Marketed Predicate Device(s)

The LZI Oral Fluid Amphetamine Enzyme Immunoassay (K131653) is substantially equivalent to the Lin-Zhi International, Inc. Oral Fluid Amphetamine Enzyme Immunoassay, Calibrators and Controls for Hitachi 717 Systems (K063024) manufactured by Lin-Zhi International, Inc. The LZI Oral Fluid Amphetamine Enzyme Immunoassay is identical or similar to its predicate in terms of intended use, method principle, device components, and clinical performance.

Device Description

The LZI Oral Fluid Amphetamine Enzyme Immunoassay is a kit comprised of two reagents, an R1 and R2 which are bottled separately but sold together within the kit.

The LZI Oral Fluid Collector is a 50 mL polypropylene collection tube. It is a non-sterile centrifuge tube with a screw-on cap and printed graduations (United Lab Plastics, Catalog#UP2262).

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Intended Use

The LZI Oral Fluid Amphetamine Controls are for use as assayed quality control materials to monitor the precision of the LZI Oral Fluid Amphetamine Enzyme Immunoassay at the cutoff value of 50 ng/mL.

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Comparison to Predicate Device

The following table compares LZI's Oral Fluid Amphetamine Enzyme Immunoassay (K131653) with the predicate device.

Device	Subject Device (K131653)	Predicate Device (K063024)
	LZI Oral Fluid Amphetamine Enzyme	LZI Oral Fluid Amphetamine Enzyme
Characteristics	Immunoassay, Calibrators and Controls	Immunoassay, Calibrators and Controls
Intended Use	The LZI Oral Fluid AmphetamineEnzyme Immunoassay, is intended for thequalitative and semi-quantitativedetermination of d-amphetamine in neathuman oral fluid, collected into the LZIOral Fluid Collector, at the cutoff value50 ng/mL. The assay is designed forprescription use with a number ofautomated clinical chemistry analyzers.This assay provides a rapid screening procedurefor determining the presence of d-amphetamine inoral fluid. The assay provides only a preliminaryanalytical result. A more specific alternativechemical method must be used in order to obtain aconfirmed analytical result. Gas or liquidchromatography/mass spectrometry (GC/MS orLC/MS) is the preferred confirmatory method.Clinical consideration and professional judgmentshould be exercised with any drug of abuse testresult, particularly when the preliminary test resultis positive.	The Amphetamine-Specific EnzymeImmunoassays for Drugs of Abuse in OralFluid is a homogeneous enzymeimmunoassay system to detectamphetamine in human saliva with acutoff of 45 ng/mL when testing oral fluidspecimen collected with Salivettecollector (manufactured by Sarstedt) anddiluted with 1 mL of buffer. Thecalibrators and controls of the analyte (d-amphetamine) are prepared with oral fluidbuffer so that it can be used to verify andvalidate the assay. The assay is intendedfor use in the qualitative determination foramphetamine. The assay is designed forprofessional use with a number ofautomated clinical chemistry analyzers.The Oral Fluid Amphetamine-Specific EnzymeImmunoassay is a homogeneous enzymeimmunoassay system provides only a preliminaryanalytical test result. A more specific alternativechemical method must be used to obtain aconfirmed analytical result. Gaschromatography/mass spectrometry (GC/MS) is thepreferred confirmatory method. Clinicalconsideration and professional judgment should beapplied to any drug-of-abuse test result,particularly when preliminary positive results areused.
Analyte	amphetamine	amphetamine
Cutoff	50 ng/ml	45 ng/mL
Matrix	Oral fluid	Oral fluid
Calibrator	5 Levels	5 Levels
Levels	(0, 25, 50, 100, 140 ng/mL)	(0, 15, 30, 45, 90 ng/mL)
Control Levels	2 Levels	2 Levels
	(37.5 ng/mL, 62.5 ng/mL)	(30 ng/mL, 90 ng/mL)
Storage	2-8 ℃ until expiration date	2-8 ℃ until expiration date

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Performance Characteristics Summary: Hitachi 717 Analyzer

50 ng/mL Cutoff Result:		Within Run		Total Precision
SampleConcentration	% of Cutoff	Number ofDetermination	ImmunoassayResult	Number ofDetermination	ImmunoassayResult
0 ng/mL	-100.0%	22	22 Negative	88	88 Negative
12.5 ng/mL	-75.0%	22	22 Negative	88	88 Negative
25 ng/mL	-50.0%	22	22 Negative	88	88 Negative
37.5 ng/mL	-25.0%	22	22 Negative	88	88 Negative
50 ng/mL	100.0%	22	11 Pos/11 Neg	88	36 Pos/52 Neg
62.5 ng/mL	+25.0%	22	22 Positive	88	88 Positive
75 ng/mL	+50.0%	22	22 Positive	88	88 Positive
87.5 ng/mL	+75.0%	22	22 Positive	88	88 Positive
100 ng/mL	+100.0%	22	22 Positive	88	88 Positive

Semi-Quantitative Positive/Negative Results:

Qualitative Positive/Negative Results:

50 ng/mL Cutoff Result:		Within Run		Total Precision
SampleConcentration	% of Cutoff	Number ofDetermination	ImmunoassayResult	Number ofDetermination	ImmunoassayResult
0 ng/mL	-100.0%	22	22 Negative	88	88 Negative
12.5 ng/mL	-75.0%	22	22 Negative	88	88 Negative
25 ng/mL	-50.0%	22	22 Negative	88	88 Negative
37.5 ng/mlL	-25.0%	22	22 Negative	88	88 Negative
50 ng/mL	100.0%	22	8 Pos/14 Neg	88	46 Pos/42 Neg
62.5 ng/mL	+25.0%	22	22 Positive	88	88 Positive
75 ng/mL	+50.0%	22	22 Positive	88	88 Positive
87.5 ng/mL	+75.0%	22	22 Positive	88	88 Positive
100 ng/mL	+100.0%	22	22 Positive	88	88 Positive

Linearity:

Hitachi 717 Instrument: 0 - 140 ng/mL

When comparing the result (y) and target (x) value, using the least squares regression technique, the regression equation and correlation are as follow: y = 1.0555x - 0.7832, r2 = 0.9945

Method Comparison: Clinical Samples

From a total of eighty-five (85) clinical unaltered samples For both Qualitative and Semi-Quantitative results: 100.0 % agreement with negative, 97.7 % agreement with positive samples

Endogenous Compound Interference and Specificity - Cross-Reactivity:

No significant undesired cross reactants or endogenous substance interference was observed. See product insert for list of compounds tested.

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Shipping/Recovery Stability Study:

No significant sample degradation occurred following real-time and accelerated stability studies up to 72 hours. All sample shipments are based on the assumption of a 24 hour priority overnight delivery.

Sample Storage Stability Study:

No significant sample degradation occurred following real-time and accelerated stability studies up to 13 Days. Based on real-time studies, samples can be stored at 2-8 ℃ for up to 13 Days. Based on the Arrhenius equation, accelerated stability data supports at least 18 months of shelflife storage at -20 ℃. Real-time stability studies are on-going.

Open (and re-capped) vial Stability for Calibrator/Control:

Real time (2 - 8 ℃) and accelerated stability studies (at room temperature and 30 ℃) were carried out for 17 months (568 Days) and results indicated degradation at all three conditions was minimal. Thermal stability data supports at least 18 months of shelf life storage at 2 - 8 ℃.

Closed Stability for Reagents Shelf-life:

Real-time stability studies were carried out for 17 months (568 Days) and results indicated degradation is minimal. Real-time stability data also supports at least 18 months of shelf life storage at 2 - 8 ℃.

Summary:

The information provided in this pre-market notification demonstrates that the LZI Oral Fluid Amphetamine Enzyme Immunoassay (K131653) is substantially equivalent to the legally marketed predicate device for its general intended use. Substantial equivalence was demonstrated through comparison of intended use and physical properties to the commercially available predicate device as confirmed by gas or liquid chromatography/mass spectrometry (GC/MS or LC/MS), an independent analytical method, The information supplied in this pre-market notification provides reasonable assurance that the LZI Oral Fluid Amphetamine Enzyme Immunoassay is safe and effective for its stated intended use.

200 - 100 - 100 .. Det 11: 11:3 : :

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DEPARTMENT OF HEALTH & HUMAN SERVICES

Image /page/6/Picture/1 description: The image shows the logo for the U.S. Department of Health & Human Services. The logo consists of a circular seal with the text "DEPARTMENT OF HEALTH & HUMAN SERVICES - USA" arranged around the perimeter. Inside the circle is a stylized symbol that resembles an eagle or bird in flight, composed of three curved lines.

Public Health Service

Food and Drug Administration 10903 New Hampshire Avenue Document Control Center - WO66-G609 Silver Spring, MD 20993-0002

February 4, 2014

LIN-ZHI INTERNATIONAL, INC. BERNICE LIN VP OPERATIONS 670 ALMANOR AVENUE SUNNYVALE CA 94085

Re: K131653

Trade/Device Name: LZI Oral Fluid Amphetamine Enzyme Immunoassay LZI Oral Fluid Amphetamine Calibrators and Controls Regulation Number: 21 CFR 862.3100 Regulation Name: Amphetamine test system Regulatory Class: II Product Code: DKZ, DLJ, LAS Dated: December 10, 2013 Received: December 12, 2013

Dear Dr. Lin:

We have reviewed your Section 510(k) premarket notification of intent to market the device referenced above and have determined the device is substantially equivalent (for the indications for use stated in the enclosure) to legally marketed predicate 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) that do not require approval of a premarket approval application (PMA). 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. Isting of devices, good manufacturing practice, labeling, and prohibitions against misbranding and adulteration. Please note: CDRH does not evaluate information related to contract liability warranties. We remind you, however, that device labeling must be truthful and not misleading.

If your device is classified (see above) into either class II (Special Controls) or class III (PMA), it may be subject to additional controls. Existing major regulations affecting your device can be found in the Code of Federal Regulations, Title 21, Parts 800 to 898. In addition, FDA may publish further announcements concerning your device in the Federal Register.

Please be advised that FDA's issuance of a substantial equivalence determination does not mean that FDA has made a determination that your device complies with other requirements of the Act or any Federal statutes and regulations administered by other Federal agencies. You must comply with all the Act's requirements, including, but not limited to: registration and listing (21 CFR Part 807); labeling (21 CFR Parts 801 and 809); medical device reporting (reporting of medical device-related adverse events) (21 CFR 803); good manufacturing practice requirements as set forth in the quality systems (QS) regulation (21 CFR Part 820); and if applicable, the electronic product radiation control provisions (Sections 531-542 of the Act); 21 CFR 1000-1050.

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If you desire specific advice for your device on our labeling regulations (21 CFR Parts 801 and 809), please contact the Division of Small Manufacturers, International and Consumer Assistance at its toll-free number (800) 638 2041 or (301) 796-7100 or at its Internet address http://www.fda.gov/MedicalDevices/ResourcesforYou/Industry/default.htm. Also, please note the regulation entitled, "Misbranding by reference to premarket notification" (21CFR Part 807.97). For questions regarding the reporting of adverse events under the MDR regulation (21 CFR Part 803), please go to

http://www.fda.gov/MedicalDevices/Safety/ReportaProblem/default.htm for the CDRH's Office of Surveillance and Biometrics/Division of Postmarket Surveillance.

You may obtain other general information on your responsibilities under the Act from the Division of Small Manufacturers, International and Consumer Assistance at its toll-free number (800) 638-2041 or (301) 796-7100 or at its Internet address

http://www.fda.gov/MedicalDevices/ResourcesforYou/Industry/default.htm.

Sincerely yours,

Courtney 2014.02.02

Courtney H. Lias. Ph.D. Director Division of Chemistry and Toxicology Devices Office of In Vitro Diagnostics and Radiological Health Center for Devices and Radiological Health

Enclosure

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DEPARTMENT OF HEALTH AND HUMAN SERVICES Food and Drug Administration

Indications for Use

510(k) Number (if known) K131653

Device Name

LZ! Oral Fluid Amphetamine Enzyme Immunoassay and LZI Oral Fluid Amphetamine Calibrators and Controls

Indications for Use (Describe)

The LZI Oral Fluid Amphetamine Enzyme Immunossay is intended for the qualitative determination of damphetamine in neat human oral fluid, collected into the LZI Oral Fluid Collector, at the cutoff value of 50 ng/mL. The assay is designed for prescription use with a number of automated clinical chemistry analyzers.

The semi-quantitative mode is for purposes of (1) enabling laboratories to determine an appropriate dilution of the specimen for confirmation by a confirmatory method such as GCMS or (2) permitting laboratories to establish quality control procedures.

The LZI Oral Fluid Amphetamine Calibrators are for use as callorators in the qualitative callbration of the LZI Oral Fluid Amphetamine Enzyme Immunoassay at the cutoff value of 50 ng/mL.

The LZI Oral Fluid Amphetamine Controls are for use as assayed quality control materials to monitor the LZI Oral Fluid Amphetamine Enzyme Immunoassay at the cutoff value of 50 ng/mL.

The assay provides only a preliminary analytical result. A more specific altemical method must be used in order to obtain a confirmed analytical result. Gas or liquid chromatography/mass spectrometry (GCMS) is the preferred confimatory method. Clinical consideration and professional judgment should be exercised with any drug of abuse test result, paticularly when the preliminary test result is positive.

Type of Use (Select one or both, as applicable)

Prescription Use (Part 21 CFR 801 Subpart D)

Over-The-Counter Use (21 CFR 801 Subpart C)

PLEASE DO NOT WRITE BELOW THIS LINE - CONTINUE ON A SEPARATE PAGE IF NEEDED.

FOR FDA USE ONLY

Concurrence of Center for Devices and Radiological Health (CDRH) (Signature)

FORM FDA 3881 (1/14)

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Regulation Number and Section

§ 862.3100 Amphetamine test system.

(a)
Identification. An amphetamine test system is a device intended to measure amphetamine, a central nervous system stimulating drug, in plasma and urine. Measurements obtained by this device are used in the diagnosis and treatment of amphetamine use or overdose and in monitoring levels of amphetamine to ensure appropriate therapy.(b)
Classification. Class II (special controls). An amphetamine test system is not exempt if it is intended for any use other than employment or insurance testing or is intended for Federal drug testing programs. The device is exempt from the premarket notification procedures in subpart E of part 807 of this chapter subject to the limitations in § 862.9, provided the test system is intended for employment and insurance testing and includes a statement in the labeling that the device is intended solely for use in employment and insurance testing, and does not include devices intended for Federal drug testing programs (e.g., programs run by the Substance Abuse and Mental Health Services Administration (SAMHSA), the Department of Transportation (DOT), and the U.S. military).