Deciding on CLL Therapy and When to Treat- ONC... - CLL Support

CLL Support

23,337 members40,042 posts

Deciding on CLL Therapy and When to Treat- ONCLive Video discussion Drs. Wierda, Lamanna, Ma, Davids, Coutre

lankisterguy profile image
lankisterguyVolunteer
11 Replies

This has been discussed often- when to start treatment. There are many exceptions and special conditions, but the only agreement is not to treat on White Blood Count.

youtu.be/A66CR1ubb-c

Transcript:

William G. Wierda, MD, PhD: So, let’s move on to treatment. We’ll start the discussion, first, talking about first-line therapy. And maybe, Matt, you can start. The iwCLL guidelines came out. The last version was in 2008 and my understanding is that there’s a new version that’s forthcoming very soon. Maybe you could just briefly review the indications to start treatment, what are we looking for, and which should be the triggers to start treatment?

Matthew S. Davids, MD, MMSc: This is fairly common if you’re familiar with indolent non-Hodgkin’s lymphoma. The criteria are similar but a little bit different in CLL. So, the iwCLL criteria, there’s 3 main groups that I cluster these into. And those include patients who are developing cytopenias that are due to infiltration of the CLL into the bone marrow. There’s different thresholds that we can use. Hemoglobin in the 10 to 11 range is where we start to think about treatment or platelets in the 100 or less range. If patients are developing bulky lymphadenopathy that’s either highly symptomatic or sometimes for cosmetic reasons if it’s in the neck, patients may want treatment. And then the third reason that’s often the most challenging is when patients are having symptoms that are being driven by CLL disease progression. And sometimes, these can be vague constitutional symptoms.

Fatigue is often a common complaint, which may sometimes be related to CLL but may be related to other medical issues. So, if fatigue alone is the presenting complaint, I usually look hard to find another cause if the CLL is not progressing. But in the context of progressive CLL, fatigue, unintentional weight loss, night sweats, and these sorts of things can all be reasons to initiate treatment. More rarely, patients can have autoimmune cytopenias. We try to treat these with steroids or rituximab. But if they’re refractory to those treatments, then sometimes full blown CLL therapy will be required.

William G. Wierda, MD, PhD: How about early treatment? Early treatment for anybody, 17p for example?

Matthew S. Davids, MD, MMSc: So, this has been studied in a number of randomized trials over the years. Most of these have looked at chemotherapy or chemoimmunotherapy-based interventions for higher-risk patients, and these studies have all been negative in terms of an overall survival benefit for early intervention.

Nicole Lamanna, MD: Or not enrolled.

Matthew S. Davids, MD, MMSc: Or not enrolled, that’s true. There’s an interesting ongoing study in Germany now, the CLL12 study, looking at early intervention with ibrutinib, but we don’t have data back from that.

Steven Coutre, MD: Again, high-risk patients.

Matthew S. Davids, MD, MMSc: And high-risk patients. So, I would not advocate early intervention outside of the iwCLL criteria.

Nicole Lamanna, MD: But an important question that hopefully will get answered with the study.

Matthew S. Davids, MD, MMSc: Yes.

Shuo Ma, MD, PhD: One other factor, too, for indication for treatment is the short lymphocyte doubling time. So, when the absolute lymphocyte doubling time is less than 6 months, that could be an indication for treatment, even though it’s kind of a soft criteria.

William G. Wierda, MD, PhD: Any white blood cell count usually it doesn’t happen in isolation. That has been my experience. Is there any white blood cell count at which point patients need to start treatment?

Shuo Ma, MD, PhD: No. So, the absolute lymphocyte count itself is really not an indication to treat. Because CLL patients—the lymphocyte’s different from acute chemotherapy, especially ALL—who have a very high number of white blood cells actually almost never see the leukostasis.

Nicole Lamanna, MD: I think that’s the one thing we do have to caution. So I agree with you. I think that you’re following the doubling time. But I think that they are different. Everybody’s tempo is different and there are some people who may rapidly rise but then plateau for a while and rise again. So, if you want to change the frequency of the visit because they are rapidly doubling, that’s fine because you’re going to try to catch them before they develop cytopenias. We have to caution physicians not to just treat based on the white blood cell count or the doubling because there could be a change of tempo, and it may be OK. You just bring them in sooner to see what’s going on.

Shuo Ma, MD, PhD: Right. And you also have to find out what’s going on with a patient otherwise. For example, I often have patients who had a steroid injection for their arthritis. And then when the next visit comes, their white blood cell count may have had a huge jump. But then you can follow them longer and they go back to their previous baseline. So don’t rush to go into treatment if it’s solely based on white blood cell counts.

Matthew S. Davids, MD, MMSc: One other nuance to that is that if you decide you want to check FISH testing at baseline diagnosis, that’s great. But if a patient goes on observation for a period of time and then has a somewhat sudden change in the rapidity of the lymphocyte doubling time, it’s important to repeat the FISH testing before you start treatment. Because actually, patients can undergo spontaneous clonal evolution to deletion 17p, and you need to know that before you start treatment.

William G. Wierda, MD, PhD: So frontline therapies become more complicated because there’s a lot more options. There are different approaches that people can take, that physicians can take, and patients also are developing their own opinions about what they want and how they want to be managed. So I think we’re going to have some relatively diverse opinions in the next discussion. I think maybe we’ll start with something that probably we’ll all agree on, and that is how to manage a previously untreated patient who has 17p deletion. I think there’s less controversy in that topic. Maybe, Dr. Ma, you can comment on how one would manage a patient with 17p deletion who needs to be treated.

Shuo Ma, MD, PhD: We know from historical data from chemoimmunotherapy that patients with 17p deletion really don’t do very well, and they either don’t respond or if they respond, they have a very short duration response. But with the new development of the BTK inhibitor, currently we have ibrutinib available, so that has definitely shown that even patients with symptom 17p deletion can equally benefit from the ibrutinib therapy. So, nowadays, I think probably most of us would agree that for a patient with 17p deletion, it’s better to avoid immunochemotherapy because not only does it not help, it actually may induce more genetic changes, which may make the disease more aggressive. Instead, those patients would be most suitable for novel kinase inhibitor therapy such as ibrutinib.

William G. Wierda, MD, PhD: Is age an important feature when you’re thinking about that patient with 17p that you’re going to start on a PTK inhibitor or…?

Shuo Ma, MD, PhD: Age will be something, yes. Whenever we start any treatment, we have to look at a patient as a whole: their age, their comorbidities. For chemoimmunotherapy, age is a huge factor. But for kinase inhibitors, age itself is really not an important factor. It’s more the comorbidities and there are other medications that will determine whether there’s any contraindication or increased risk for taking ibrutinib.

William G. Wierda, MD, PhD: So, in terms of the non-17p deletion, maybe we can start with you, Steven. You can comment on what are the features and characteristics that you consider when you’re considering first-line therapy for a patient. What’s important and how do you use that information in your approach?

Steven Coutre, MD: Again, to emphasize, if you haven’t tested for prognostic reasons, this is the time to test mutation status, repeat the FISH. And in many circumstances, particularly as Matt mentioned, it’s sudden change. So, that’s really important because now we’re talking about predictive factors in some cases. And then, of course, the fitness of the patient, however you want to measure that. I think we all can tell after a few minutes talking to our patients whether they tolerate a chemoimmunotherapy regimen. And then, I think a really, really important point is, what’s your goal? What is your goal in that individual patients?

If you’re starting therapy because somebody is 78 and they’ve got bulky neck and head neuropathy, they may tell you, “I don’t want to lose my hair,” and that’s their main goal. And that’s very different than how you might approach somebody who’s 68 who has got cytopenias and bulky disease. So, take all that information, decide what you want to achieve because it’s not one-size-fits-all.

But I think one really important issue is mutation status. It’s clear, repeatedly, that chemoimmunotherapy regimens do not give prolonged benefit in the unmutated patient. And of all the tests that we do, that’s the one that probably is done least often. You can see a lot more FISH testing, which is great. So, that’s really, really important. The kinase inhibitors work equally as well whether you’re mutated or unmutated in contrast to chemoimmunotherapy. If you’re looking at a young patient, let’s say, that’s really important because you might consider chemoimmunotherapy in a fit patient or at least have that conversation with them if they’re mutated. Whereas if they’re unmutated, perhaps, right now we have ibrutinib commercially available. And in the older patients, for tolerability reasons, you might easily just choose ibrutinib. But again, we have obinutuzumab if you want to use an antibody to shrink lymph nodes in an elderly person, that’s your goal. And some people may still want to give bendamustine and rituximab in select patients. So, it sort of depends. But at least we have information to allow us to make choices.

William G. Wierda, MD, PhD: So, repeating FISH and mutation status, those are the 2 lab tests that are most useful in directed therapy and not considering the patient’s age and comorbidities.

Matthew S. Davids, MD, MMSc: IGVH mutations, just to be clear.

Steven Coutre, MD: Yes.

Matthew S. Davids, MD, MMSc: IGVH mutation status.

Steven Coutre, MD: Readily available tests.

Nicole Lamanna, MD: Agreed.

Transcript Edited for Clarity

Len

Written by
lankisterguy profile image
lankisterguy
Volunteer
To view profiles and participate in discussions please or .
Read more about...
11 Replies

Interesting but also a bit contradictory. They know giving patients chemotherapy with 17p is bad in terms of short remissions but also can make the disease more aggressive but wouldn’t that be the case with most patients without the desired 13q deletion and mutated status?

Also there discussing doubling ALC times in regard starting treatment but then saying sometimes they can just level off and decline, I wonder if there are other factors in play once Cll becomes active such as stress or exposure to poor diet or environmental issues that people avoid once there diagnosed and without knowing there bodies sort of go into repair mode.

I know Cll is caused by a weakness in the immune system which could be any of the above or just a decline due to the ageing process which is why it used to be called a disease in the elderly but more younger people seem to be developing it now so lifestyle factors must come into play. The foods we eat are mass produced and full of sugars and chemicals the water we drink is full of chemicals and the air we breath is slightly toxic not to mention the stresses of life ie financial worries and how fast paced things are now.

Stuart

lankisterguy profile image
lankisterguyVolunteer

Hi Lewis78,

Since your are in the UK, your NHS wants to give everyone Chemo except those with 17p.

All the doctors in the video are in the USA and their expressed opinions seem to disagree with your NHS. They indicate that they would NOT give Chemo to anyone UnMutated regardless of deletions, and if you asked them they probably will avoid Chemo for 11q and Normal. That would mean that the only patients that would be offered Chemo are 13q Mutated and Tri 12 Mutated, and some USA doctors (like Dr. Furman) will not give Chemo to any patients.

The remainder of your questions have lots of hypothetical "what ifs". I have witnessed both Dr. Lamanna and Dr. Coutre answering those, and I believe they will answer that the patient and the doctor must decide based on the exact conditions of the patient at that moment and that patient's history.

In the video Dr. Lamanna talks about increasing the frequency of exam appointments when the "tempo" of ALC rise is rapid, she specifically excluded using doubling time as a reason to treat. So she gets more data points to determine if someone plateaus, but also detects if the patient is getting into dangerous territory with Red Blood components ( Hgb, Hct & platelets) or Neuts.

So deciding to treat is very complicated and has little science and lots of art.

Len

in reply tolankisterguy

Hi Len

I think what I wrote came across the wrong way, I didn’t mean the people on that panel were contradictory, I meant leading specialists around the world discuss the latest developments and treatments and must know now giving chemotherapy to patients other than those with the desired genetics can cause secondary mutations and alter the landscape of there disease.So why is the risk still being taken.

Given the opportunity I would drop my haematologist in the U.K. and be taken under care by Dr Lammana immediately,I’ve been following some of her posts since I first got diagnosed and she is one of the most passionate caring physicians in the Cll world.

Stuart

in reply tolankisterguy

How are you getting on with your treatment.

lankisterguy profile image
lankisterguyVolunteer in reply to

I'm fine, was MRD neg for most of 2017, paused Venetoclax in Sept, but my MRD test went from 0 to 100 in 4 months, so I restarted Ven in January. All my blood tests are normal as they have been for nearly 2 years. No side effects, no issues. Genentech sends me a new bottle every month- no charge. Life is wonderful.

Len

in reply tolankisterguy

That’s good news then! I’ve read some very encouraging posts in regards Venetoclax especially in combinations.

Do you think you hadn’t been taking it long enough to cause a deep enough remission?

It’s good news you get it without charge! Are you part of a trial? Do you think it could become a lifelong therapy for you like Ibrutinib.

Stuart

lankisterguy profile image
lankisterguyVolunteer in reply to

I am not in a trial, it was offered, but I opted not. My first trial 2012-2105 included 4-5 CT Scans per year, and the Ventoclax trial had similar frequency. I don't want to glow in the dark or get more skin cancer, so until they back off on the radiation, I won't join if I can get the drugs another way.

As for all your other questions, Dr. Furman answers those with "We just don't have the data" or "We just don't know".

Len

in reply tolankisterguy

Yes I’ll second your thoughts on the scans, I’m part of a trial with Ibrutinib/Rituximab and have had two so far but plan on trying to avoid any more or if possible just opting for an MRI.

Good luck and hopefully soon you can discontinue taking the Venetoclax and get a longer deeper remission.

Stuart

lankisterguy profile image
lankisterguyVolunteer in reply to

Hi Stuart,

I have heard that some Clinical Trials allow a patient to start and use MRI's but none that were allowed to switch in the middle.

I talked to my clinical trial doctor and he advised me confidentially that I could refuse every other scan, and the trial coordinator from the drug company would not object strenuously, but if I refused more than that, they would likely remove me from the trial. (The doctor said he could not actively disclose his advice, but if I independently refused, he would remain passive- the clinical nurses and staff that were not involved were alarmed when i took my stance, but when there were no repercussions, they all calmed down).

This got me down to 2 scans per year- and when I compared the dose data- it was less than the radiation allowed for US-NRC workers in nuclear plants. nrc.gov/about-nrc/radiation...

Len

in reply tolankisterguy

Hi Len

I’ve done the same as you and asked before my previous CT about refusing it to my haematologist and I pretty much got the same reply that I might get kicked off the trial.

Although being part of a trial means your a bit of lab rat! I think you do have to be proactive and put your own health first sometimes. I know now they sometimes use CT scans unnecessarily and I’m sure I read somewhere somebody avoided one on their clinical trial and had an MRI but I’m going to do everything possible to avoid my next one unless there’s a valid reason for me needing it.

I know frequent flying exposes you to a higher doses of radiation and as you’ve said above two scans a year equals lower than that of workers on nuclear plants but we do need to avoid any unnecessary exposure.

Do you live in the city itself or a borough outside? I went to New York in 2007 and it’s an amazing city, learnt a lot about heights from the top of the Empire State Building.

Stuart

Jem67 profile image
Jem67

Thanks for posting that, Len. As you say there is a lot of art involved when making a decision about when to start treatment and that is why, we as patients should be fully involved and not passive.

Also, can Doctors realy tell whether patients will tolerate chemo by talking to them for a few minutes?! I don' t think so.

Joy

Not what you're looking for?

You may also like...

Acalabrutinib Plus Venetoclax and Obinutuzumab Achieves High Bone Marrow uMRD Rate in Chronic Lymphocytic Leukemia - CLL

Great news from this long awaited first published phase 2 study reporting the efficacy of this AVO...
AussieNeil profile image
Partner

Untreated CLL with 17 p deletion

Hi, l need some advise. I was diagnosed 6 years ago with CLL. I have been in W&W until recently my...
Anita1 profile image

Practicing with the Patient Voice: A Patient Decision Library: Wow! 4 patient stories/ Drs. Anthony Mato + Dr. Matt Davids comment

Practicing with the Patient Voice: A Patient Decision Library: Wow! There is only one thing more...
bkoffman profile image
CLL CURE Hero

Zanubrutinib vs. Ibrutinib Patient Power Video by Dr. Jennifer Brown MD PHD

In this Patient Power video - Dr. Brown is very clear about the advantages of Zanubrutinib over...
lankisterguy profile image
Volunteer

Median PFS for FCR treated CLL patients with IGHV-M was 14.6 years vs 4.2 years for patients with IGHV-UM. V+O and I+R look to be superior

An update of the long-term follow-up results from the original 300-patient FCR (fludarabine,...
AussieNeil profile image
Partner

Moderation team

See all
Newdawn profile image
NewdawnAdministrator
AussieNeil profile image
AussieNeilAdministrator
CLLerinOz profile image
CLLerinOzAdministrator

Content on HealthUnlocked does not replace the relationship between you and doctors or other healthcare professionals nor the advice you receive from them.

Never delay seeking advice or dialling emergency services because of something that you have read on HealthUnlocked.