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PlasmaSEQ Overview

Myeloma has long been hindered by poor risk stratification and limited testing capabilities as FISH is highly dependent on sample transport and manual processes.

PlasmaSEQ addresses this by enabling testing with as little as 1 nanogram per microliter of DNA, ensuring that physicians can obtain the maximum amount of information from minimal biological material.

Additionally, since PlasmaSEQ is a DNA-only assay, it is more resilient to environmental stresses and the logistical challenges of sample transport.

With > 500X depth targeted coverage PlasmaSEQ detects mutations in clones as low as 1.3%*

Why PlasmaSEQ

1st Global NGS-based test for Myeloma

Validated for DNA input per sample of as low as 10 ng

1000 Samples validated in 3 countries with 95% accuracy*.

Rapid turnaround time

One stop test for detecting all genomic events including biallelic somatic changes

PlasmaSEQ

Del (17p)

Del (1p32)

1q21 amplification/gain

IGH Translocations

t(4;14)IGH::FGFR3

t(14;16)IGH::MAF

t(11;14)IGH::CCND1

t(6;14)IGH::CCND3

t(14;20)IGH::MAFB

TP53 Mutation

BRAF V600E

All RAS/RAF Mutations

DIS3-DEL(13q) Mutation

SLAMF7, BCMA & APRIL* and GPRC5D

Genomic Profiling of ATM

Trisomies & Hyperdiploidy 
across the genome

FISH

Del (17p)

Del (1p32)

1q21 amplification/gain

IGH Translocations

t(4;14)IGH::FGFR3

t(14;16)IGH::MAF

t(11;14)IGH::CCND1

t(6;14)IGH::CCND3

t(14;20)IGH::MAFB

*To be released in upcoming Plasmaseq 2.0

FAQ's

Minimum sample: 2 ml of EDTA-Bone Marrow
PlasmaSEQ is a comprehensive, all-in-one solution for Multiple Myeloma cases. This next-generation sequencing (NGS) method offers an extensive genomic overview, covering IGH translocations, mutations, amplifications, Trisomies & Hyperdiploidies. It eliminates the need for multiple assays such as karyotyping and FISH, while providing in-depth insights.
PlasmaSEQ checks Bi-allelic deletions (CDKN2C), multi-exonic (TP53) deletions that are missed by FISH and helps determine the course of targeted therapy (Immunotherapy).
PlasmaSEQ can perform testing with as little as 1 nanogram per μL of DNA, ensuring that physicians obtain the maximum amount of information from low sample volume.