BTKi in R/R CLL and MCL

CME

A Global Perspective on Emerging BTK Inhibitor Therapy Data for Relapsed/Refractory CLL and MCL in 2022

Physicians: Maximum of 1.00 AMA PRA Category 1 Credit

Released: December 16, 2022

Expiration: December 15, 2023

Othman Al-Sawaf
Othman Al-Sawaf, MD
Matthew S. Davids
Matthew S. Davids, MD, MMSc
Toby A Eyre
Toby A Eyre, MBChB, MD
Christopher R. Flowers
Christopher R. Flowers, MD, MS
Brad S. Kahl
Brad S. Kahl, MD
Kami Maddocks
Kami Maddocks, MD
Anthony Mato
Anthony Mato, MD, MSCE
Lydia Scarfò
Lydia Scarfò, MD
Julie M. Vose
Julie M. Vose, MD

Activity

Progress
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Course Completed
BRUIN CLL/SLL: Faculty Discussion from Pan Pacific Lymphoma Conference

Matthew S. Davids, MD, MMSc:
The phase I/II BRUIN study evaluated pirtobrutinib (formerly LOXO-305) in patients with CLL/SLL or B-cell non-Hodgkin lymphoma following treatment with at least 2 prior therapies, including a BTK inhibitor.8 Of the 618 patients included, 261 patients with CLL were evaluated. A very impressive response was seen in this study, with an ORR of 68%. This is remarkable considering there really isn’t a standard of care approach for these patients. Also presented was an impressive waterfall plot that highlighted the point that patients—whether they had discontinued their previous BTK inhibitor due to progression or toxicity—had an equal response to pirtobrutinib. The response was observed across different risk groups, including patients who have the classic BTK inhibitor resistance mutation BTK C481S. It is particularly interesting that these patients responded equally well to pirtobrutinib compared with patients who did not. This drug really has potential in either group of patients.

Matthew S. Davids, MD, MMSc:
Finally, the safety profile of pirtobrutinib looks very good, and in patients with CLL, this was a well-tolerated drug. We did see some of the typical BTK inhibitor–related toxicities such as bruising, although typically low grade, with very low rates of more major bleeding and background incidence of atrial fibrillation and hypertension. There were no dose-limiting toxicities. They did not reach a maximum tolerated dose, so 200 mg was selected as the dose moving forward. I think it’s exciting, as we think about where the relapsed CLL field is heading, to know that phase III studies are now launching with pirtobrutinib compared with standards of care. Hopefully, this will eventually lead to an FDA approval for pirtobrutinib in relapsed/refractory CLL.

Julie M. Vose, MD, MBA:
The toxicity profile does look good for pirtobrutinib. Assuming the future phase III trials show similar outcomes and, in addition, demonstrate the ability to overcome some of the resistance issues, where do you think pirtobrutinib will sit in the future as far as therapy for our patients with CLL?

Matthew S. Davids, MD, MMSc:
That’s a crucial question, and they also are launching registrational trials for pirtobrutinib in the frontline setting. These studies, fortunately, will take a long time, as patients with CLL generally do well for a longer time. I think it is going to be difficult to supplant the covalent BTK inhibitors. We certainly know, right now, that the sequence of starting with a covalent BTK inhibitor and then moving to pirtobrutinib is successful, but it’s going to take several years before we have the opposite order, where we start with pirtobrutinib and then need to know whether covalent BTK inhibitors can be effective subsequently. From early reports, it does seem that a different pattern of resistance mutations is arising with the noncovalent inhibitors, and whether the covalent BTK inhibitors can overcome that remains an open question. But, to your point, because the toxicity profile of pirtobrutinib does look so good, if that really holds up in the phase III experience, it could be a best-in-class molecule and used in the frontline setting based on the safety and efficacy profile.

SEQUOIA: Frontline Zanubrutinib vs Bendamustine/Rituximab in Patients with CLL/SLL and No del(17p)

Matthew S. Davids, MD, MMSc:
SEQUOIA is a phase III study of zanubrutinib, another covalent BTK inhibitor that is not yet approved in CLL.14,15 SEQUOIA included multiple cohorts, but the one I think will be most impactful is cohort 1, the registrational cohort where patients were randomized to receive continuous zanubrutinib or a standard 6-month course of BR. This was an older CLL population with a median age of approximately 70 years and various risk markers. This cohort excluded high-risk patients with del(17p).

SEQUOIA (Cohort 1): IRC-Assessed PFS (Primary Endpoint)

Matthew S. Davids, MD, MMSc:
At 24 months, the data look very good for zanubrutinib. It is a relatively early look for a frontline CLL study, but nonetheless at 24 months there was an 85% PFS rate with zanubrutinib compared with approximately 70% with BR. This benefit was observed across different risk groups based on genetics and various clinical characteristics. The one group without a significant improvement in PFS was patients with mutated IGHV CLL, where there was a numerical but not yet statistically significant advantage for zanubrutinib. That’s to be expected with short follow-up, and these patients can do well with BR.

 

SEQUOIA (Cohort 1): AEs of Interest

Matthew S. Davids, MD, MMSc:
The safety profile continues to look very good for zanubrutinib, with very few patients needing to discontinue due to toxicity, but there are some risks around neutropenia and hypertension with zanubrutinib. Looking at the adverse event data, in a randomized comparison of zanubrutinib and BR, most striking was that the rates of atrial fibrillation were equivalent between the 2 arms—in the range of approximately 3%—and that has not been observed with the other BTK inhibitors, including ibrutinib or acalabrutinib, where we typically see a higher rate of atrial fibrillation in these randomized comparisons with chemoimmunotherapy. Again, this is a short follow-up, and it will be interesting to see if any differences emerge over time, but it is very encouraging from a safety perspective.

SEQUOIA (Cohort 1): Discussion

Matthew S. Davids, MD, MMSc:
I think one question that will arise is: How are we going to use zanubrutinib in CLL once it is approved by the FDA? We’ll have 3 great options in the frontline setting—acalabrutinib, ibrutinib, and zanubrutinib—and these also will be options in the relapsed setting. The bottom line is that it’s good for patients to have choices. All of these drugs have somewhat different adverse event profiles, and we’ll probably be using all three in clinical practice.

Julie M. Vose, MD, MBA:
Yes, that’s a good point. In what particular patient profile would you tend to shy away from ibrutinib and go toward some of these newer BTK inhibitors?

Matthew S. Davids, MD, MMSc:
For me, the older patients—particularly those with comorbidities that involve cardiovascular disease—are the ones where I’m avoiding ibrutinib now, because we have head-to-head phase III data comparing acalabrutinib vs ibrutinib and zanubrutinib vs ibrutinib, and to me the takeaways from those studies are that, particularly for patients with cardiovascular comorbidities, this next generation of covalent BTK inhibitors is better tolerated. I think there are still young, fit patients who can tolerate ibrutinib well—and it is once-daily dosing, and there’s a very long track record with the drug and a lot of experience—so there is an opportunity for those patients. For the decision between acalabrutinib and zanubrutinib, we do have patients, for example, who suffer from headaches. That is a known risk with acalabrutinib, so that might be a patient for whom you’d prioritize zanubrutinib. We may have patients who have issues with hypertension, and it seems like the rates are a little higher with zanubrutinib, so maybe we start that patient on acalabrutinib. Various other nuances between these drugs might push us one way or the other.

Julie M. Vose, MD, MBA:
Yes, absolutely. I think the other issue to bring up is that hypertension with ibrutinib happens sometimes very late, and you have to continue to monitor patients carefully. I’ve seen the hypertension happen years later, and it can sneak up on you, and you have to be careful about that. So that’s another patient population where you may want to change to a different BTK inhibitor.

MAJIC: What Is the Optimal Venetoclax-Based Doublet for Frontline CLL Treatment?

Matthew S. Davids, MD, MMSc:
Lastly, I want to mention the MAJIC trial, which is trying to answer the question of: What is the optimal venetoclax-based doublet for frontline CLL treatment across all-comers, all ages, and all genetic risk groups? (NCT05057494) This trial has not yet activated but is a comparison of the standard comparator arm of venetoclax and obinutuzumab with a combination of acalabrutinib and venetoclax. This is a noninferiority study with a primary endpoint of 3-year PFS.

One thing that is unique about this study is that both arms have MRD-guided treatment duration. Typically, the venetoclax plus obinutuzumab approved regimen is 1 year for all patients regardless of their MRD status at the end of that year. To make this a fairer comparison, both arms are allowing a measurement of MRD at the end of 1 year of venetoclax. Those patients who are undetectable for MRD would stop treatment, and those who still have detectable MRD would go on to receive a second year of venetoclax. Of importance, as we move toward more time-limited therapies in CLL, all patients in the MAJIC study will stop treatment after 2 years of venetoclax-based therapy regardless of their MRD status at that time.

Another unique aspect of this study is that we’re using the next-generation sequencing–based approach clonoSEQ for our MRD testing. This is allowing us to get down to a level of 10-5 detection consistently rather than 10-4 by flow cytometry, which has traditionally been used in trials. The hope is that this will allow for more accurate risk stratification and identification of patients who can safely discontinue therapy and enjoy a long PFS.

Any patient with CLL in need of frontline treatment who is a candidate for venetoclax should be eligible for this study. One situation where they may not be a great candidate is in the setting of significant renal dysfunction. But this trial has broad eligibility, and we anticipate it will recruit relatively quickly.

Over time, we will see if differences emerge. Another key question that this study will help address is: Is it worth it to use the BTK inhibitor early on, or is it better to save it for later?

BRUIN-MCL-321: What Is the Optimal BTK Inhibitor for Pretreated BTK Inhibitor–Naive MCL?

Julie M. Vose, MD, MBA:
BRUIN MCL-321 is large, international phase III trial of approximately 500 patients in a 1:1 randomization of pirtobrutinib vs choice of the other BTK inhibitors—acalabrutinib, ibrutinib, or zanubrutinib—in patients with previously treated MCL who have not received a prior BTK inhibitor. Basically, it is evaluating the first BTK inhibitor for this patient population. This is a very important study for seeing if pirtobrutinib is better as far as outcomes and toxicity and then, of course, for looking at the mutations of MCL to see if there’s a particular patient population for which pirtobrutinib would be better. This trial just started, and although it’s going to be a long time before we get answers to these questions, it is an important one to discuss with our patients.

Matthew S. Davids, MD, MMSc:
Do you think they’re looking at the right endpoints on this trial? Is it going to give us meaningful data?

Julie M. Vose, MD, MBA:
It is. They’re looking at response rates, PFS, and OS. It’s going to be unlikely, at least in the short term, that there will be an OS advantage; these patients would likely need to be followed for a very long time to see that. But certainly, response rates and PFS are important endpoints, and then of course tolerability, as well. And then looking at the time of relapse—if they do get mutations, too. So, yes, I think there are good endpoints. This is an important study, and I’ll be interested to see the results.

Matthew S. Davids, MD, MMSc:
Yes, certainly I will, as well. Also, the safety comparison is going to be interesting because we don’t have randomized data comparing pirtobrutinib with other BTK inhibitors, and I wonder whether we’ll extrapolate from this MCL study into CLL if we do see meaningful safety differences among the different drugs.

Which of the following patients with MCL would be eligible for enrollment on the phase III BRUIN-MCL-321 trial?
BRIDGE: Zanubrutinib-Based Induction and Maintenance in Untreated MCL

Julie M. Vose, MD, MBA:
The BRIDGE trial is an interesting study. This study includes patients with MCL with no central nervous system involvement and no prior stem cell transplant who receive induction with R-CHOP for 3 cycles, alternating with R-DHAP or similar regimens for 3 cycles every 21 days, and also receive zanubrutinib on cycles 1, 3, and 5 with the R-CHOP regimen. Then, if the patients have PR or better they can go on to autologous stem cell transplant per standard of care. As part of the study, they receive zanubrutinib maintenance for 2 years after the transplant. The primary endpoint is MRD negativity, and secondary endpoints are PFS and OS.

A small initial subset of this study was presented at the 2022 Pan Pacific Lymphoma Conference. It included 7 patients with a median age of 52 years and mostly advanced-stage disease, as would be expected. All patients had peripheral blood and bone marrow involvement, as well as some with gastrointestinal and other involvement, which is typical for MCL. This is a short follow-up—a median of only 35 weeks—but they were able to complete MRD testing in the majority of patients and found that, in 5 of the 7 who had completed at least 1 MRD test, all had achieved MRD negativity in the peripheral blood and bone marrow. One patient had gone on to stem cell transplant.

As far as safety, the majority of patients tolerated zanubrutinib very well without any major adverse events or complications. Grade 3/4 neutropenia was found in only 2 of the 7 patients with zanubrutinib.

Although these data are very early, it is a really interesting analysis and design. I think this is something we’re going to see a lot more of—the different combinations of chemotherapy, immunotherapy, and BTK inhibitors together.

Matthew S. Davids, MD, MMSc:
Yes, for sure. One of the things that seems appealing to me about this design is that it’s a time-limited amount of a BTK inhibitor after those 2 years of maintenance.

Julie M. Vose, MD, MBA:
Yes, the study design is a 2-year, time-limited BTK inhibitor, which again I think is an important aspect because, unfortunately, the BTK inhibitors are expensive, and to receive these agents for an unlimited number of years can be difficult for patients, including from a toxicity standpoint. So, the time-limited aspect is very important.

Matthew S. Davids, MD, MMSc:
Yes, I agree. It also might open up using the BTK inhibitor again as another line of therapy if they have several years of remission. So, there are lots of potential advantages there.

Julie M. Vose, MD, MBA:
Yes, to have the ability to somewhat mix and match our different treatments. To have time off therapy may mean the lymphoma becomes sensitive again to that particular agent or a similar agent. So, particularly with the BTK inhibitors, that’s an important concept.