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PMC Hereditary Lymphoma Panel

Up to 43 genes Turn around Time: 10 business days

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Test Description

PMC Hereditary Lymphoma Panel analyzes genes linked to a hereditary predisposition to lymphoma. Due to the genetic diversity associated with lymphoma| relying solely on phenotype can be challenging in pinpointing the exact cause. Testing a broad panel of genes allows for a more efficient evaluation of potential genetic factors associated with lymphoma. This test specifically targets heritable germline mutations and does not detect somatic mutations.

Patient (Consult a Provider) Provider

Associated Conditions
- Autoimmune lymphoproliferative syndrome
- Genes associated with susceptibility to EBV and lymphoproliferative conditions, and lymphoma as a feature
- Genes associated with immune dysregulation and lymphoma as a feature
- Constitutional mismatch repair deficiency syndrome (CMMR-D)

Methodology

Targeted Exome/ Slice Exome (Next Generation Sequencing including Copy Number Variation)

Coverage

120x

Assay Information
- PTEN: Sequencing analysis for exons 8 includes only cds +/- 10 bp.
- BRCA1: Sequence analysis includes +/- 20 base pairs of adjacent intronic sequence.
- BRCA2: Sequence analysis includes +/- 20 base pairs of adjacent intronic sequence.
- ACAN: Sequencing analysis is not offered for exon 12.
- MLH1: Deletion/duplication analysis covers the promoter region. Sequencing analysis for exons 12 includes only cds +/- 10 bp.
- MSH6: Sequencing analysis for exons 7| 10 includes only cds +/- 10 bp.
- TP53: Deletion/duplication analysis covers the promoter region.
- ATM: Sequencing analysis for exons 6| 24| 43 includes only cds +/- 10 bp.
- MSH2: Analysis includes the exon 1-7 inversion (Boland mutation). Sequencing analysis for exons 2| 5 includes only cds +/- 10 bp. Deletions restricted to only the EPCAM gene will not be detected unless EPCAM analysis is requested.
- PMS2: Sequencing analysis for exons 7 includes only cds +/- 10 bp.
- EPCAM: Sequencing analysis is not offered for this gene.
- NF1: Sequencing analysis for exons 2| 7| 25| 41| 48 includes only cds +/- 10 bp.

Ordering information

Turnaround Time: 10 business days

Preferred Speciment: Saliva Kits (available upon request)

Alternate Specimens: Nail clippings or 3-mL whole blood in purple top EDTA tube

Request a specimen collection kit

Limitations

All sequencing technologies have limitations. A negative result from this analysis does not rule out a possible genetic diagnosis as some variants may not be detected by this test. This test is not designed to detect low level mosaicism, structural rearrangements, indels >40bp, deep intronic variants of unknown clinical significance, or large cytogenetic CNVs. Certain inherent qualities of the human genome, for example repetitive regions/homopolymers, GC rich, pseudogenes, and rare polymorphisms, pose significant technical challenges such as sequence misalignment that may potentially impact the accuracy of the results. False negative results may also occur in the setting of allogeneic bone marrow, stem cell transplantation, active or chronic hematologic conditions, recent blood transfusions, suboptimal DNA quality or PCR trace contamination. Other potential sources of error include sample mix-ups and clerical issues.

References
- 1. Richards S et al. Genetics in medicine. Standards and guidelines for the interpretation of sequence variants: a joint consensus recommendation of the American College of Medical Genetics and Genomics and the Association for Molecular Pathology. 2015 May;17(5):405-24 (PMID: 25741868)
- 2. GnomAD (gnomAD)
- 3. CSPEC (ClinGen variant classification rules registry) Criteria Specification Registry
- 4. Normal copy number variation in healthy individuals database of genomic variants: http://dgv.tcag.ca/dgv/app/home
- 5. Riggs, E.R., Andersen, E.F., Cherry, A.M. et al. Technical standards for the interpretation and reporting of constitutional copy-number variants: a joint consensus recommendation of the American College of Medical Genetics and Genomics (ACMG) and the Clinical Genome Resource (ClinGen). Genet Med 22, 245–257 (2020). https://doi.org/10.1038/s41436-019-0686-8
- 6. Landrum MJ, Lee JM, Riley GR, Jang W, Rubinstein WS, Church DM, Maglott DR. ClinVar: public archive of relationships among sequence variation and human phenotype. Nucleic Acids Res. 2014 Jan 1;42(1):D980-5. doi: 10.1093/nar/gkt1113. PubMed PMID: 24234437.
- 7. Online Mendelian Inheritance in Man, OMIM®. McKusick-Nathans Institute of Genetic Medicine, Johns Hopkins University (Baltimore, MD), Copyright® 1966-2012. World Wide Web URL: http://omim.org.
- 8. http://tinyurl.com/ACMGv4 (ACMG/ Clingen draft Interpretation SOP); clingen_variant-curation_sopv1.pdf

Tagged Genes

Primary panel:

43 genes selected

ADA ATM BLM CARD11 CARMIL2 CASP8 CD27 CTLA4 CTPS1 DOCK8 EPCAM FADD FAS FASLG FCHO1 IKZF1 IL2RA IL2RB ITK MAGT1 MCM4 MLH1 MSH2 MSH6 NBN NF1 PIK3CD PIK3R1 PMS2 PRKCD RAC2 RASGRP1 RHOH RMRP SH2D1A STAT3 STK4 STXBP2 TNFRSF13B TP53 TPP2 WAS XIAP

Based at Germantown Innovation Center (GIC) in Maryland, USA. Precision Medicine Care (PMC®) employs state of art technologies to deliver advanced clinical genomic diagnostic testings. Our clinical laboratory is accredited by CAP and licensed by CLIA for performing high complexity tests.

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