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Printable Handouts
Navigable Slide Index
- Introduction
- Rational combination strategies in RR MM
- POM, bortezomib & PVd vs. bortezomib & Vd
- Progression-free survival (ITT)
- Progression-free survival (1 prior line of therapy)
- Conclusions and future directions
- Elotuzumab + EPD vs PD
- Demographics and baseline characteristics
- Progression-free survival (ITT definition)
- Progression-free survival
- Progression-free survival: prior lines of therapy
- Overall response rate and best overall response
- Preliminary overall survival
- Conclusions
- Venetoclax+ carfilzomib & dexamethasone
- Background
- Study design and patient enrolment
- Objective responses in all patients
- Objective responses in patients
- STORM study
- Selinexor mechanism of action
- Efficacy subgroups
- Progression free and overall survival
- Conclusions
- Key targets in MM 2019 (2)
- Melflufen therapy
- Melflufen – a novel targeted alkylating peptide
- Melflufen/dex in relapsed and refractory (RR) MM
- OP-106 HORIZON
- Prior treatment and refractory characteristics
- Best M-protein response
- ORR in multi-refractory RRMM patients
- Progression-free survival
- PFS by response category
- HORIZON: patient case
- Conclusions and future directions
- Key targets in MM 2019 (3)
- Overcoming the tumour
- Isatuximab can directly kill CD38 MM cells
- Isa diminishes Tregs while activates effector cell
- Isatuximab in relapsed/refractory myeloma
- Antibody drug conjugates
- Anti-BCMA antibody drug conjugate
- BCMA CAR-T cell trials summary
- CAR T – progression-free survival in RR MM
- CAR T - bb2121 adverse events of special interest
- 2nd gen. BCMA-targeted CAR T-Cell therapy
- Additional CAR T-Cell therapy strategies
- BCMA-BiTE-based immunotherapies
- AMG 40
- Background
- Study schematic/objectives
- CRS AEs and serious AEs (SAEs)
- Responding patients’ characteristics
- Conclusions
- Key features of vaccine design
- Cell-based myeloma vaccines
- PVX-410 multi-peptide vaccine study
- Integration and impact of novel agents in RR MM
- The impact of novel therapies in MM ~ 2019
- Continuing evolution of MM treatment
- Thank you
Topics Covered
- T-cell therapy strategies for Multiple Myeloma
- Cell-based Myeloma vaccines
- Antibody-drug conjugates
- Continuing evolution of Multiple Myeloma treatment
Talk Citation
Richardson, P.G. (2019, June 30). The evolving role of novel and next generation therapies in the management of multiple myeloma: relapse refractory multiple myeloma 2 [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved December 30, 2024, from https://doi.org/10.69645/FUWQ5129.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: relapse refractory multiple myeloma 2
Published on June 30, 2019
19 min
A selection of talks on Cancer
Transcript
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0:05
Now, for the last part of my presentation,
I want to move into the space of relapsed refractory disease.
I'll move through this relatively promptly for you in the interests of time.
Rational combination strategies are in
the treatment of the relapsed refractory myeloma are critical.
With the advent of novel agents third generation IMiDs,
next generation proteasome inhibitors of monoclonal antibodies,
the playing field has been dramatically changed.
0:30
Now, I want to share with you some of the data from
the combination of pomalidomide, bortezomib,
and dexamethasone compared to a control of
bortezomib and dexamethasone relapsed refractory disease.
This is the so-called OPTIMISMM trial which we presented first at ASCO in last year,
and then this was updated most recently by my colleague,
Dr. Thanos Dimopoulos, at the ASH meeting this last December.
0:53
Progression-free survival by intent to treat was strikingly in
favor of the three drugs over the two with hazard ratio of 0.61.
1:01
But what's really interesting is if you looked at one prior line of therapy,
and importantly in this study,
all the patients were lenalidomide exposed,
and 70 percent of them were in fact lenalidomide refractory.
If you look at the first relapse group,
what we were very pleased to see was despite lenalidomide exposure and/or refractoriness,
the pomalidomide, bortezomib, dexamethasone platform generated
a median progression-free survival to 21 months with a hazard ratio of 0.54.
What was particularly also important,
was that in this context,
the safety signal was excellent.
So this constitutes something that I think is very important for our patients,
1:38
that essentially when lenalidomide treatment has failed a patient,
we have excellent options that are pomalidomide based,
and also potentially affordable because
they incorporate bortezomib which is now generic as
the proteasome inhibitor platform combined with the
two to generate the powerful three-drug platform.
So the OPTIMISIMM data are quite exciting.
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