The xTAG® Gastrointestinal Pathogen Panel (GPP) is a multiplexed nucleic acid test intended for the simultaneous qualitative detection and identification of multiple viral, bacterial and parasitic nucleic acids in human stool specimens or human stool in Cary-Blair media from individuals with signs and symptoms of infectious colitis or gastroenteritis. The following pathogen types, subtypes and toxin genes are identified using the xTAG GPP:

Viruses

• · Adenovirus 40/41
• · Norovirus GI/GII
• · Rotavirus A

Bacteria

• · Campylobacter (C. jejuni, C. coli and C. lari only)
• · Clostridium difficile (C. difficile) toxin A/B
• · Escherichia coli (E. coli) O157
• · Enterotoxigenic E. coli (ETEC) LT/ST
• · Salmonella
• · Shiga-like Toxin producing E. coli (STEC) stx 1/stx 2
• · Shigella (S. boydii, S. sonnei, S. flexneri and S. dysenteriae)
• · Vibrio cholerae (V. cholerae) cholera toxin gene (ctx)

Parasites

• · Cryptosporidium (C. parvum and C. hominis only)
• · Entamoeba histolytica (E. histolytica)
• · Giardia (G. lamblia only, also known as G. intestinalis and G. duodenalis)

The detection and identification of specific gastrointestinal microbial nucleic acid from individuals exhibiting signs and symptoms of gastrointestinal infection aids in the diagnosis of gastrointestion when used in conjunction with clinical evaluation, laboratory findings and epidemiological information. A gastrointestinal microorganism multiplex nucleic acid-based assay also aids in the detection of acute gastroenteritis in the context of outbreaks.

xTAG GPP positive results are presumptive and must be confirmed by FDA-cleared tests or other acceptable reference methods.

The results of this test should not be used as the sole basis for diagnosis, treatment, or other patient management decisions. Confirmed positive results do not rule out co-infection with other organisms that are not detected by this test, and may not be the sole or definitive cause of patient illness. Negative xTAG GPP results in the setting of clinical illness compatible with gastroenteritis may be due to infection by pathogens that are not detected by this test or non-infectious causes such as ulcerative colitis, irritable bowel syndrome, or Crohn's disease.

xTAG GPP is not intended to monitor or guide treatment for C. difficile infections.

The xTAG GPP test is indicated for use with the Luminex® 100/200™ and MAGPIX® instruments with xPONENT® software.

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The provided text is a 510(k) clearance letter for the xTAG Gastrointestinal Pathogen Panel (GPP) and xTAG Data Analysis Software (TDAS GPP). While it details the "Indications for Use" and general regulatory information, it does not contain the specific technical acceptance criteria, study details, or performance data for the device.

Therefore, I cannot provide the requested information based on the given input.

To answer your request, I would need a section of the document that describes the clinical performance study, often found in a "Performance Data" or "Clinical Study Results" section of a 510(k) submission. This section typically includes:

• Acceptance Criteria: Predetermined performance targets (e.g., sensitivity, specificity, positive predictive agreement, negative predictive agreement thresholds).
• Reported Device Performance: The actual sensitivity, specificity, and other metrics achieved by the device in the study.
• Study Design: Details about the sample size, data provenance, ground truth establishment, and any comparison to predicate devices or reference methods.

Without this information in the provided text, I am unable to populate the table or answer the specific questions about the study design.