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Printable Handouts
Navigable Slide Index
- Introduction
- Targeting kinases in the BCR pathway
- Activated BCR signaling in CLL
- The BCR signal transduction pathway
- BCR pathway inhibition in CLL
- BTK as a target in B cell malignancies
- Ibrutinib (PCI-32765): BTK inhibitor
- PCYC-1102/1103 phase 2 study design
- 1102: response over time
- 1102 best response (Investigator-assessed)
- Patient disposition (36 mo F/U)
- 1102 PFS by cytogenetics (FISH) in R/R CLL
- OS by cytogenetics (FISH) in R/R population
- PCYC-1112 RESONATE study design
- Ibrutinib and Ofatumumab: PFS
- PFS for Ibrutinib with or w/o lymphocytosis
- PFS for Ibrutinib with or w/o Del17p
- Gene mutation characteristics
- PFS and ORR by gene mutation at baseline
- RESONATE: treatment discontinuation
- RESONATE: progressive disease
- Safety: atrial fibrillation and adverse events
- Ibrutinib discontinuation for non-PD by age
- Time to discontinuation
- Survival after discontinuing Ibrutinib
- Survival: progressive CLL v. Richter’s
- Patients with identified mutations at relapse
- Conclusions: Ibrutinib (1)
- Conclusions: Ibrutinib (2)
- PI3K signaling pathway as a target in B cells
- Idelalisib is highly selective for PI3K delta
- Nodal and overall response rate
- Gilead study 116: R-Idela vs R-placebo
- Key eligibility for Gilead study
- PFS, Idelalisib + Rituximab vs. placebo + Rituximab
- PFS subgroup analysis Idelalisib + Rituximab
- Laboratory abnormalities of interest
- Phase 2 single arm, open label study
- Response assessment
- Idelalisib + Rituximab in untreated CLL over 65
- Adverse events leading to discontinuations
- Idelalisib PFS
- Summary: Idelalisib
- Venetoclax (ABT-199): mechanism of action
- ABT-199 dosing schema
- Best change in lymphocytes and nodal mass
- Best percent change in bone marrow infiltrate
- Objective responses of ABT-199 treated patients
- PFS at 400 mg or higher
- Dosing schedule of Venetoclax and Rituximab
- Responses by subgroup
- Bone marrow minimal residual disease (MRD)
- Durability of responses after Venetoclax
- CLL therapy, ca early 2015
- Ongoing clinical trials in CLL
- Open questions (1)
- Open questions (2)
Topics Covered
- Relapsed therapy in CLL
- Targeted therapy
- BTK inhibition
- PI3K delta inhibition
- Clinical trials (initial vs. relapsed)
Talk Citation
Brown, J.R. (2015, November 30). CLL: novel prognostics, and updates on therapy 2 [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved December 26, 2024, from https://doi.org/10.69645/UTCV5704.Export Citation (RIS)
Publication History
Financial Disclosures
- Prof. Jennifer R. Brown has not informed HSTalks of any commercial/financial relationship that it is appropriate to disclose.
CLL: novel prognostics, and updates on therapy 2
Published on November 30, 2015
35 min
A selection of talks on Haematology
Transcript
Please wait while the transcript is being prepared...
0:04
That section of the talk
summarized the current standard
of care for initial therapy
in both fit and
unfit CLL patients.
Now I'm going
to turn my attention
primarily to relapse therapy,
but also primarily
to the targeted therapies
of the B-cell receptor pathway
which have been
recently approved in CLL
and are generating
so much excitement.
And so in this slide
we see a schematic
of the B-cell receptor pathway,
as well as some
of the drugs targeting
different proteins
in this pathway
that have been tested
in the last number of years.
Some of their early
studies tested Dasatinib
as a potential LYN inhibitor.
And more recently,
Dasatinib has also been shown
to have activity against BTK.
Fostamatinib is
a SYk inhibitor
and Everolimus
is an mTOR inhibitor.
And these studies all had
fairly modest activity in CLL.
Nothing that exciting.
The first drugs to generate
a huge amount
of excitement were Idelalisib,
the inhibitor
of PI3-kinase delta.
And again the delta isoform
is most critical in CLL cells.
And Ibrutinib, the BTK inhibitor.
There have of course, now also
been subsequent generations
of PI3-kinase and BTK inhibitors
that have moved
into clinical trials.
Listed some of them here.
Idelalisib, XL147 which is
a pan-PI3-kinase inhibitor
that's been tested.
IPI 145 is a gamma delta
PI3-kinase inhibitor.
Gamma's also
found in neutrophils
and T cells
as well as CLL cells.
So this may add efficacy
but may also add toxicity.
That drug is currently
in registration trials.
And for BTK inhibitors
the CC-292 drug
has been tested,
ONO-4059 has been tested,
and now also ACP-196
is moving rapidly
into registration trials.
I will focus
most of my discussion
today on Idelalisib
and Ibrutinib
and then we'll also talk
about BCl2 inhibition,
as that looks like the next drug
to be approved
in all likelihood.