ExPeCT™ anti-CD19 (liso-cel) CAR T-cell Assay

Test Code: 33597

Understanding the limitations of anti-CD19 (liso-cel) CAR T cell therapy is critical to realizing the full potential of this treatment approach. Growing experience with these agents has revealed that remissions will be brief in a substantial number of patients owing to poor CAR T cell persistence and/or cancer cell resistance resulting from antigen loss or modulation. The Viracor ExPeCT anti-CD19 (liso-cel) CAR T expansion and persistance assay is a monitoring tool to evaluate and validate the efficacy of anti-CD19 CAR T therapy.

CAR T Chimeric Antigen Receptor

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Clinical and Procedure
Clinical Utility

Monitoring for expansion and persistence of CAR T-cells (liso-cel) after infusion. Loss of CAR T persistence may indicate relapse or recurrence of leukemia in patients administed CAR T-cell immunotherapy.

About Test

The successes with chimeric antigen receptor (CAR) T cell therapy involving patients with pre-B cell acute lymphoblastic leukaemia (ALL) or B cell lymphomas have revolutionized anticancer therapy, providing a potentially curative option for patients who are refractory to standard treatments. FDA approvals of anti-CD19 CAR T (liso-cel) cell product for both ALL and certain types of B cell lymphoma. CD19-targeted CAR T cells, which have been engineered to recognize the CD19 cell surface molecule of malignant B cells. Some patients relapse due to the CAR T therapy not persisting in the body, leading to antigen loss or tumor escape. Growing experience with these agents has revealed that remissions may be brief in a substantial number of patients owing to poor CAR T cell persistence.

Procedure

Extraction of genomic acid from whole blood specimen followed by PCR amplification of CAR and Rnase P targets using real-time PCR methods. An internal control is added to ensure that extraction was performed correctly and that the PCR reaction was not inhibited.

Specificity

Inclusivity: liso-cel prepared from multiple donors, specificity: human genomic DNA, FMC63 scFv DNA

Turnaround Time

24 hours from receipt of specimen, performed Monday - Saturday

Specimen Information
Specimen Type Test Code CPT Code NY Approved Volume Assay Range Special Instructions
whole blood 33597 80299 Yes

2.0 mL (min 0.5 mL)

N/A
  • Collect 2.0 mL whole blood in EDTA tube
  • Ship at frozen temperature Monday through Friday for overnight delivery
Shipping

Ship Monday through Friday. Friday shipments must be labeled for Saturday delivery. All specimens must be labeled with patient's name and collection date. A Eurofins Viracor test requisition form must accompany each specimen. Ship specimens FedEx Priority Overnight® to: Eurofins Viracor, 18000 W 99th St. Ste. #10, Lenexa, KS 66219

Causes for Rejection

Specimens beyond their acceptable length of time from collection as listed in the specimen handling.

Disclaimer

Specimens are approved for testing in New York only when indicated in the Specimen Information field above. The CPT codes provided are based on Eurofins Viracor’s interpretation of the American Medical Association's Current Procedural Terminology (CPT) codes and are provided for informational purposes only. CPT coding is the sole responsibility of the billing party. Questions regarding coding should be addressed to your local Medicare carrier. Eurofins Viracor assumes no responsibility for billing errors due to reliance on the CPT codes illustrated in this material.

References
  1. JHOP - February 2022 Vol 12, No 1 - Review Article, CAR T-Cell Therapy, Lymphoma Drew A. Wells, PharmD, BCPS; Jenna Summerlin, PharmD; Zachery Halford, PharmD, BCOP, BCPPS
  2. Strategies to enhance CAR‑T persistence. Yue Liu1†, Lingna An1†, Ruihao Huang1†, Jingkang Xiong, Haoyu Yang, Xiaoqi Wang and Xi Zhang Liu et al. Biomarker Research (2022) 10:86 Liu et al. Biomarker Research (2022) 10:86 https://doi.org/10.1186/s40364-022-00434-9
  3. Safarzadeh Kozani P, Safarzadeh Kozani P and Rahbarizadeh F (2021). Optimizing the Clinical Impact of CAR-T Cell Therapy in B-Cell Acute Lymphoblastic Leukemia: Looking
    Back While Moving Forward. Front. Immunol. 12:765097. doi:0.3389/fimmu.2021.765097
  4. Developing and Monitoring a Standard-of-Care Chimeric Antigen Receptor (CAR) T Cell Clinical Quality and Regulatory Program. https://doi.org/10.1016/j.bbmt.2020.03.021 1083-8791/© 2020 American Society for Transplantation and Cellular Therapy. Published by Elsevier Inc.
  5. Jafarzadeh L, Masoumi E, Fallah-Mehrjardi K, Mirzaei HR and Hadjati J (2020) Prolonged Persistence of Chimeric Antigen Receptor (CAR) T Cell in Adoptive Cancer Immunotherapy: Challenges and Ways Forward. Front. Immunol. 11:702. doi:10.3389/fimmu.2020.00702
  6. CAR-T Cells: The Importance of Cell Persistence. Sep 13, 2021| Russell Garland https://www.frontiersin.org/articles/10.3389/fimmu.2020.00702/full
  7. The Leukemia & Lymphoma Society. Immunotherapy Facts. https://www.lls.org/booklet/immunotherapy. Revised December 2019. Accessed October 19, 2021
  8. National Cancer Institute. CAR T cells: engineering patient’s immune cells to treat their cancers. https://www.cancer.gov/about-cancer/treatment/research/car-t-cells. Updated: July 30, 2019. Accessed October 20, 2021.
  9. Brodsky AN. The promise of CAR T cell therapy in 2019 and beyond. Cancer Research Institute [website]. https://www.cancerresearch.org/blog/september-2019/promise-car-tcell-therapy-2019-beyond. Accessed October 15, 2021. https://www.cancer.gov/about-cancer/treatment/research/car-t-cells
  10. Sanber, K., Savani, B. and Jain, T. (2021), Graft-versus-host disease risk after chimeric antigen receptor T-cell therapy: the diametric opposition of T cells. Br J Haematol, 195: 660-668. https://doi.org/10.1111/bjh.17544
  11. CAR-T cell therapy: practical guide to routine laboratory monitoring. Adrian G Selim, Adrian Minson, Piers Blombery, Michael Dickinson, Simon J Harrison, Mary Ann Anderson.
    Pathology. 2021 Apr;53(3):408-415. doi: 10.1016/j.pathol.2021.02.002. Epub 2021 Mar 5.
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