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Printable Handouts
Navigable Slide Index
- Introduction
- Disclosures
- Multiple myeloma…not just one disease!
- Multiple myeloma is highly complex disease
- Interaction between plasma cells & bone marrow
- Multimodality targeting of MM
- Multiple options are now available to treat
- Multiple Myeloma is a marathon, not a sprint
- Key targets in MM, 2019 (1)
- Principles of initial therapy in SCT eligible ND MM
- A model for treating SCT-eligible MM patients
- Lenalidomide/Bortezomib-based Rx in NDMM
- RVd vs Rd in Patients Without Immediate Intent
- IFM2009: RVd alone vs RVd + ASCT
- IFM/DFCI 2009: response
- Summary of Lenalidomide maintenance
- Lenalidomide maintenance post-transplant
- Ixazomib
- Progression Free Survival (PFS)
- PFS subgroup analysis
- Response rates and MRD status
- Updates on the use of next-generation agents
- Carfilzomib-lenalidomide-dexamethasone
- Trial design
- Aims of the current analysis
- Patients characteristics
- Response rate after ASCT or 8 KRd cycles
- Response rate pre-maintenance (1)
- Response rate pre-maintenance (2)
- MRD rate pre-maintenance
- Safety (1)
- Safety (2)
- Conclusions
- Griffin study
- Daratumumab
- GRIFFIN: safety run-in phase (N = 16)
- Efficacy: investigator-assessed response rate
- MRD negativity (10–5; ITT) and outcomes
- Conclusions
- GRIFFIN randomized phase 2 study design
- MRD assessment
- MRD assessment via NGS
- IFM/DFCI 2009: importance of treatment arm
- Future directions for ND MM/ ASCT candidates
- Phase 3 DETERMINATION study
- BMT CTN protocol 1401
- DETERMINATION 2
- A cautionary note
- Summary in ND MM +/- ASCT
- Treatment options for ND MM/ non- ASCT
- Lenalidomide, bortezomib and dexamethason
- RVD lite: schema
- RVD lite: baseline characteristics
- RVD lite: safety – grade 3 or greater toxicity
- RVD lite: patient-reported outcomes
- RVD lite: conclusions
- phase 3 of D-rd
- MAIA study design
- Efficacy: PFS
- Efficacy: ORRa and MRDb _x000B_
- Efficacy: PFS by MRD status
- Efficacy: OS at median follow-up of 28 months
- Conclusions
- Phase 1 of Vrd
- Targeting CD38 with Isatuximab
- Patient demographics and clinical characteristics
- Response summary (IMWG criteria)
- Minimal residual disease evaluation
- Conclusions
Topics Covered
- Multiple myeloma and key targets in 2019
- Principles of initial therapy in stem cell transplant
- Therapeutics and drug agents used in Multiple Myeloma
Links
Categories:
Therapeutic Areas:
Talk Citation
Richardson, P.G. (2019, June 30). The evolving role of novel and next generation therapies in the management of multiple myeloma: introduction and current therapies 1 [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved December 26, 2024, from https://doi.org/10.69645/TTJO3667.Export Citation (RIS)
Publication History
Financial Disclosures
- Advisory board member for: Celgene Corporation, Novartis, Takeda, Oncopeptides, Amgem. Recipient of research funding from: Celgene, Takeda, Oncopeptides, Bristol-Myers Squibb.
The evolving role of novel and next generation therapies in the management of multiple myeloma: introduction and current therapies 1
Published on June 30, 2019
37 min
A selection of talks on Oncology
Transcript
Please wait while the transcript is being prepared...
0:00
Hello. My name is Dr. Paul Richardson.
I'm the RJ Corman Professor of Medicine at Harvard Medical School,
and I serve as the Clinical Program Leader and Director of
Clinical Research at the Jerome Lipper Multiple Myeloma Center,
Dana-Farber Cancer Institute in Boston, Massachusetts.
It's my pleasure to talk to you today about
the evolving role of novel and next-generation therapies
in multiple myeloma and to share with you today
current status and future directions in our field.
0:27
First, I want to show you my next slide,
which simply is disclosures.
These are my relevant disclosures to the discussion
today and reflect my service on advisory committees,
as well as research funding.
0:40
Now, in the context of multiple myeloma it's
important to recognize that this is not just one disease.
Clearly, multiple myeloma as it sounds is many different diseases.
There's enormous variance between patients and, in fact,
within a patient, disease can change over time.
This recognition of what we call clonal heterogeneity has been
essential in our understanding of what we call risk stratification.
Fortunately, with the advent of novel therapies over the last three decades,
there's been an ability to individualize treatment.
1:12
So as we consider the complexity of multiple myeloma biology,
it's very important to appreciate that not only is
multiple myeloma truly multiple and what
that means is very traumatically between patients,
but it's also important to appreciate that it varies and ebbs and flows and
changes within a patient during the course of the natural history of the disease,
and in this slide I seek to capture that by illustrating to
you the clonal evolution and the matched genetic events
that myeloma evolves from its precursor states of MGUS and
smoldering disease to active disease and then to its relapsed refractory form.
Then the far right of the slide,
I really wanted to emphasize here,
and I think quite seminal work from my colleague Dr. Nikhil Munshi
looking at whole genome sequencing in the top slide of one of our patient's diagnosis.
As you can see, there are 5,000 mutations in this patient's disease at that time.
This patient then undergoes induction remission treatment,
autologous transplant, consolidation, and maintenance and then relapses.
As you can see in the bottom slide, at relapse,
the patient is challenged by 12,000 mutations in his disease.
This I think points to
the extraordinary mutagenic thrust of this illness and how we need to understand
better all the clinical implications of
such genetic instability and what that means for a patient over time,
especially as we now blessed fortunately with
multiple new treatments and modalities that can hopefully improve outcome.
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