Technology ID
TAB-3968

Molecular Classification of Primary Mediastinal Large B Cell Lymphoma Using Formalin-Fixed, Paraffin-Embedded Tissue Specimens

E-Numbers
E-172-2017-0
E-172-2017-1
Lead Inventor
Staudt, Louis (NCI)
Co-Inventors
Rimsza, Lisa (Mayo Clinic Arizona)
Scott, David (British Columbia Cancer Agency)
Wright, George (NCI)
Mottok, Anja (British Columbia Cancer Agency)
Steid, Christian (British Columbia Cancer Agency)
Jaffe, Elaine (NCI)
Gascoyne, Randy (British Columbia Cancer Agency)
Guerri, Elias (August Pi i Sunyer Biomedical Research Institute (IDIBAPS))
Guerri, Elias (Hospital Clinic de Barcelona)
Guerri, Elias (University of Barcelona)
Rosenwald, Andreas (University Of Wurzburg)
Fu, Kai (University of Nebraska Medical Center)
Greiner, Timothy (University of Nebraska Medical Center)
Smeland, Erlend (Oslo University Hospital)
Delabie, Jan (Oslo University Hospital)
Braziel, Rita (Oregon Health and Science University (OHSU))
Chan, Wing (City of Hope Medical Center)
Song, Joo (City of Hope Medical Center)
Weisenburger, Dennis (City of Hope Medical Center)
Ott, German (Robert Bosch Stiftung)
Cook, James (Cleveland Clinic)
Applications
Diagnostics
Therapeutic Areas
Oncology
Development Stages
Pre-clinical (in vivo)
Lead IC
NCI
ICs
NCI

Primary mediastinal B-cell lymphoma (PMBCL) is an aggressive type of non-Hodgkin lymphoma that mostly occurs in people between the ages of 30-40. It accounts for 5-7% of all aggressive lymphomas. The diagnosis of PMBCL is challenging as the histological features of PMBCL overlap with diffuse large B-cell lymphoma (DLBCL), another most common type of non-Hodgkin lymphoma. Available evidence suggests that PMBCL responds much more favorably to the DA-EPOCH-R chemotherapy regimen than to the standard R-CHOP regimen used to treat DLBCL. The diagnostic uncertainty of PMBCL can result in delayed and/or inappropriate treatment, serious harm, and even death of the patient, so there is a need to more precisely diagnose PMBCL.  

Researchers at the National Cancer Institute (NCI) have developed a gene expression-based assay comprising a set of 58 nucleic acid probes that measure the abundance of selected mRNA species using the Nanostring platform. This assay can be used successfully to better distinguish PMBCL from DLBCL and applied to further classify DLBCL into well-established cell-of-origin subtypes. This test can be applied by clinicians to support the pathological diagnosis of PMBCL, and therefore identify a group of patients whose tumors are characterized by a distinct underlying biology.  

The NCI seeks licensees and/or co-development partners to develop this technology toward commercialization.

Competitive Advantages:

  • Easy to integrate into current clinical practice of cancer diagnosis as the assay can be performed using routinely available formalin-fixed, paraffin-embedded (FFPE) biopsies
  • Superior prognostic ability over traditional histopathological diagnosis

Commercial Applications:

  • Diagnosis of PMBCL
  • Distinguishing PMBCL from DLBCL
  • The invention could be used: 
    • in the near term as a clinical tool in the initial diagnostic evaluation of suspected PMBCL, which is required in the WHO guidelines for diagnosis of hematologic malignancies
    • as an entry criterion for clinical trials in order to include those patients for which the efficacy of a given treatment likely depends on the molecular subtype of their disease 
  • Targeted therapies appropriate for each DLBCL subtype

Request More Info

Licensing Contact:
Bhattacharya, Ramona
ramona.bhattacharya@nih.gov

Patents

  • US
    Provisional (PRV) 62/519,728
    Filed on 2017-06-14
  • Patent Cooperation Treaty
    (PCT) PCT/US2018/036084
    Filed on 2018-06-05
  • European Patent
    National Stage 18733500.5
    Filed on 2020-01-14
  • US Patent 11,646,099
    Filed on 2019-12-13
  • France
    European patent (EP) 18733500.5
    Filed on 2020-01-14
  • Germany
    European patent (EP) 18733500.5
    Filed on 2020-01-14
  • United Kingdom
    European patent (EP) 18733500.5
    Filed on 2020-01-14

Publications

Collaborations

  • Licensing
  • Collaboration
Date Published
Date Updated