Fighting two cancer battles in one - brain and body - 1264234

louisb,

I'm truly sorry that I don't think any of the faculty can offer a suggestion of what to do in a situation in which there isn't any remote hint of evidence to suggest how to proceed, nor is there even any evidence that can even inform the potential suggestions.

As you have almost certainly learned, leptomeningeal carcinomasis is very difficult to treat effectively. We haven't seen any evidence yet about whether AZD9291 or other third generation EGFR TKI therapies have efficacy against leptomeningeal carcinomasis, but I would be very surprised if emerging phase II or III trials permit patients with LMC to enroll. If there is a compassionate use program in the future, there probably won't be any rigid eligibility requirements.

Sorry we can't offer any recommendations of how to proceed in this setting.

Good luck.

-Dr. West

Hello Louis,

I am very sorry to hear of your wife's situation; it is very similar to that of my late wife, who also had brain mets, lepto and progression in the liver and many bones. We also tried pulsed Tarceva, although this was in 2011 when pulsing was fairly new and the dosage was 600 mg every four days. And we were also faced with the issue of trying to control cancer in the CNS as well as progression in the rest of the body.

The important difference is that pulsed Tarceva seems to be working for your wife. Although as Dr. West has said there is simply not enough evidence to be able to choose a definitive treatment in such a situation, my personal, non-medical opinion would be that I would be extremely hesitant to switch away from a treatment that is currently effective. As Dr. West said, there aren't any established treatments for lepto, only anecdotal evidence of the effectiveness of pulsing Tarceva, at least for some patients. In addition, many drugs are thought to penetrate the BBB to a certain extent, but the evidence is limited and such drugs may not penetrate the BBB in sufficient concentrations to be effective. That's the theory behind pulsing Tarceva - get enough of the drug into the CNS to have efficacy.

Good luck with the treatment plan you choose.

JimC
Forum moderator

Louis,

Thank you for your kind thoughts. Yes, I did (and continue to) love Liz very much.

I assume that Lynda lost her hair due to WBRT rather than Iressa or Tarceva. Carbo/alimta doesn't tend to cause hair loss, and that was true for Liz, So that may not be a factor.

But you are correct that carbo/alimta will likely add to her fatigue. I understand that since Lynda has not had traditional chemo (including a platinum agent), he is recommending a standard platinum doublet, which would tend to provide the best response (first-line chemo agents are more effective in combination with platinum). But another option would be single-agent alimta, which is often used in (and is FDA-approved for) second-line therapy. Of course you could try the doublet and if the side effects are unmanageable drop the carbo.

JimC
Forum moderator

In the absence of both any evidence to shape a decision and a legal restriction against making medical recommendations to people who are not my patient, I am not able to suggest a treatment approach. Like Jim, however, I am very reluctant to disrupt a treatment approach that is producing good results in favor of one with many unknowns. I am especially wary about doing that in the setting of a good result in a situation in which disease control is uncommon to rare.

Good luck.

-Dr. West

Hi Louis,

That's not really true. The percentage you quote is the approximate response rate from clinical trials, often defined as either complete disappearance of the tumor being measured or shrinkage of 50% or more. But more than 30% of patients receive a benefit, as Dr. West has stated:

"When I provide estimates for what patients might expect from first line chemo for advanced NSCLC, I generally say that the response rate for significant tumor shrinkage is in the 30-35% range (40% is a tad on the high side), with another 40-45% demonstrating stable disease or perhaps mild shrinkage. Because the cancer would almost always grow as a default plan, this combined 70-75% “disease control rate” that includes those patients with stable disease or significant tumor shrinkage likely represents the proportion of patients who benefit at least a little, if not a lot, from chemotherapy." - http://cancergrace.org/topic/efficacy-of-carboalimta#post-1263654

JimC
Forum moderator

I would also add that even if you go by "response rate" and formally call it 30-35%, if that's the best odds of any of the alternatives, it's the strongest choice.

I'll also add that high dose Alimta (pemetrexed) has been compared to standard dose Alimta and shown to lead to no improvement in efficacy compared with standard dose Alimta, but greater side effects. Because of this work, there has been very little impetus for high dose Alimta in treating lung cancer (or any other cancer thus far).

-Dr. West

Just want to send my best wishes for whatever path you choose...

Louis,

I think cancer is THE suckiest point of life!!!! It was the last thing on my mind at my husband's dx. I thought(or at least hoped I guess) his symptoms were caused by something more manageable.

Yes, losing a loved one and especially a spouse, is a definite life changer! I truly thought mine was over until Jim replied to me here on GRACE. He is a very great guy and I feel truly blessed to have connected with him and have him become a part of my life and that of my kids as well. With none of his own, that has also been a life changer for him. Especially with one in her teens :wink:

May you and Lynda enjoy all of your sunrises and sunsets together.

Hi Louis,

I understand your concern about your oncologist and these "uncharted waters". One of the strengths of online forums, especially the faculty-moderated forum here at GRACE, is that information on newer treatment strategies such as pulsed Tarceva can be shared. One result is that sometimes a highly-motivated patient or caregiver (like you) can uncover ideas with which many oncologists have little or no experience.

Though trials document the most common side effects of a particular drug, patients' responses vary quite a bit, so overall toxicity is really just a patient-to-patient matter. If side effects become unmanageable, doses can be reduced or in a multi-drug regimen one or more drugs may be withheld.

Having seen the effects of lepto, and knowing how difficult it can be to find an effective treatment for it, I would repeat my personal reluctance to tamper with it, instead perhaps fine-tuning the carbo/alimta by modifying dosages, lengthening the cycle or dropping the carbo. The nature of the unmanageable symptom(s) may also suggest the remedy - if blood counts drop to unacceptable levels, the problem is most likely the chemo, since Tarceva usually does not affect blood counts. Other problems such as diarrhea or fatigue may be connected to Tarceva and adjusting its dosage might be considered. (One factor to note about Tarceva is that it has a half-life of only 36 hours, so if you're having a problem with it, modifying or delaying it can produce faster results than changing a chemo regimen).

Good luck with carbo/alimta.

JimC
Forum moderator

Hi Louis. . .

I just wanted to join the chorus in wishing your wife luck with whatever path you all choose. . .

Laya

I want to wish you luck but also to reiterate that I don't believe there is any evidence anywhere on the planet to say what to do. Neither I nor any of the other faculty can offer a suggestion when there's just no results available on what to expect. These are just completely uncharted waters, so we're left with just best judgment, and I truly can't say what I would do or favor.

Good luck.
-Dr. West

Louis, I want to join in with the others on wishing your wife the best.
Take care, Judy

Yes, please let us know how things are going.

Good luck with the addition of the chemo.

-Dr. West

Louis,

I posted this in another thread:

Tarceva can cause loss of appetite and so can radiation, especially if it touched part of the GI tract. Whatever the cause, there are a number of ways to try to combat it. Taking your anti-nausea medication on a schedule, rather than waiting for nausea to develop first, can be very effective. Also, eating smaller, snack-size meals is better than larger meals, and you may need to experiment to find foods that are appealing (and you may need to think outside the box; a number of GRACErs have settled in on some pretty strange choices!) Drinking Ensure (or a similar product) can help, as can appetite stimulants such as Megace.

GRACE member Debra (double trouble) had these suggestions:

“I will add to the applause for Ensure. I tried the other brands and they all taste like vitamins. Ensure is the only one I like. They have several flavors, and now there is a Clear Ensure that is like fruit juice. I’ve tried the apple and it’s not bad. Sometimes you just don’t want a shake.

My appetite has been turned on by some meds, off by others, and when it is pretty normal I have that heightened sense of smell/taste too.

I stick to mostly fruits and veggies, some grains like kinoa and bulgar wheat, and I need more protein but I’m a little turned off by meats, beans and eggs. Used to love them all but having trouble digesting them now.

I also find that the most simply prepared foods are the best for me. The more fussy, the less I seem to like it.

Also, you might consider a protein powder in smoothies or juices. It does have a flavor all its own so you probably either like it or you don’t, but I have lived on smoothies at times. My favorite, ginger peach!” – http://cancergrace.org/topic/tarceva-and-appetite#post-1256689

You might also want to check out these posts:

http://cancergrace.org/forums/index.php?topic=11387.0

http://cancergrace.org/forums/index.php?topic=5464.0

JimC
Forum moderator

Louis,

Unfortunately, with an advanced cancer, and probably especially with leptomeningeal disease, I don't think there's likely to be a clear answer to her difficulty with eating and weight loss. It is very much part of the whole difficult picture that makes it such an infamously difficult complication.

-Dr. West

louisb, I don't want to try to give advice, you didn't ask for any. I just wanted to send my heart out to you, Lynda and the kids. Cancer is such an awful awful disease. I hope she gets some stability back in the next days.

I've kept up with your thread and want to add my husband as an example of drinking ensure. It's probable you already have since I've written so much about it (I should get an endorsement contract). D has always been a very thin person. One of those who didn't bulk out in their twenties but always in excellent shape and good health, a one man cabinet shop keeper. In the past 5 years he never put back on the weight he lost from tumor burden, surgery, tx, et al. Chalk it up to just one of the many ways he's an outlier in the cancer world but he never got his appetite back and still relies on Ensure Plus when he can't eat. One of the lessons I've learned was to not push food on him, it makes him feel bad that he's not able to eat. Dr. West has said that a symptom like cachexia isn't as difficult for the person with it as we caregivers might think. Sometimes fantasy and bs are good medicines. Another part of learning began with this piece, http://cancergrace.org/coping-with-cancer/2009/04/29/denial-coping-mech…

So there, no advice right? humph sure. :wink:

Janine

I'm afraid that with the leptomeningeal disease, she's likely to be on a tightrope where even the slightest additional challenge will knock her off. The chemo isn't typically that difficult, but even leptomeningeal carcinomatosis alone can completely disable people.

Good luck.

-Dr. West

Louis,

Leptomeningeal carcinomatosis is also known as carcinomatous meningitis. Meningitis is an inflammation of the meninges, which include the tissue of the spinal cord. In the case of LMC, it is the cancer which causes that inflammation, rather than an infection. I would think that LMC is the likely cause of her symptoms and spinal cord inflammation.

I certainly understand how you are both feeling, and the dilemma you face about whether to continue treatment.. My wife did not want to discontinue her treatment, and though I knew we had reached the point at which it was extremely unlikely to help, we did continue for a time beyond that point. When it became clear that it was only making a bad situation worse, we had a frank conversation with her oncologist and shifted our focus to doing everything we could to make her as comfortable as possible. Though at first she was angry and depressed, she quickly accepted the decision and seemed relieved to know that she would not be faced with the awful symptoms of LMC for an extended period of time. I can't say whether that time has come for you and Lynda but I hope that when it does the two of you can find a way to accept it peacefully.

JimC
Forum moderator

I suspect her issues are most likely attributed to the cancer within her nervous system (LMC), but her doctors would have a better chance of addressing this question.

-Dr. West

Dear Louisb

I want to join the chorus of others on Grace to wish you and Lynda my hopes and prayers in her battle with LMC. 1500 MG pulse doses is the highest I have heard anywhere yet. My wife, Beth, pulse dosed 900MG and that was considered very high just last year. I fear the paralysis in her legs is from the LMC. That was the first serious symptom Beth experienced once she was diagnosed. Don't be surprised if incontinence follows. I think you are right inj staying with the current program. Beth was also taking Alimta. along with the Tarceva. You two are in a horrible situation, I don't know how else to say it. LMC really sucks and it is unrelenting. I do believe the high doses of Tarceva have kept her going this long and her progress may be studied by other docs and patients. I also hope the insurance industry follows her case too because here in the states 30 tablets a month (4500 MG) is all they will approve.

Please get yourself some help and do not let her try to get out of bed alone no matter how good she feels. I also suggest you get a portable commode and keep it in her room. I would also recommend that you start looking into hospice so you can make an informed decision at the right time. I sure don't want to sound like the Grinch who stole Christmas, and I pray for both of you that she is as fortunate as Valerie Harper, but your last post has got me concerned.

I have not been as regular on Grace since I went back to work last month, but I promise to be here for you if you have any questions about symptoms. God bless you and Lynda.

LouisB

This is strictly my opinion rather than advice. Based upon your wife's recent symptoms it appears that the benefits of Tarceva are beginning to diminish. Lynda has little to lose and possibly something to gain by going on the trial. Whatever decision you make will be the correct one and she will have many people praying for her. Bob

I don't have an answer to the truly unanswerable question of how best to oproceed, but I sincerely hope she has a better time moving forward, and I do think that AZD9291 is an appealing consideration if things are getting worse.

As for the terrible challenge of women getting lung cancer out of the blue, I wish we understood why women seem to be at higher risk for lung cancer. If we could figure out why some are prone to a genetically driven (associated with an identifiable driver mutation like EGFR, ALK, ROS, etc.) we could preselect which people should undergo screening. Otherwise, screening never-smokers or those with minimal smoking history, or younger than 55 or so are overwhelmingly likely to have any nodules detected on chest CT represent a false positive rather than real cancer that screening isn't really feasible unless we can identify the right high-risk population on which to focus.

Good luck.

-Dr. West

Hi Louis,

In April of this year, in response to a similar question regarding AZD 9291 and brain metastases, Dr. West stated:

"I don’t believe I’ve seen any results to speak to this yet. This isn’t meant to imply yes or no. I don’t think that there have been enough people tested who have known brain metastasis to present an opportunity to determine an answer to the question." - http://cancergrace.org/topic/azd-9291-and-brain-mets#post-1263246

Good luck with the new drug!

JimC
Forum moderator

I can't speak to what to expect, but I wish her and your family luck on the trial. Please keep us posted!

I would just caution that as regards to the pulsed Tarceva (erlotinib), I don't think it's a great idea to presume that more and more and more -- the most treatment that can possibly be tolerated without dying from the treatment -- isn't necessarily the best way to proceed. I would be very uncomofrtable giving way more than has every been safely administered before, or trying a combination that has never been safely given and presuming that it will be well tolerated.

Good luck.

-Dr. West

Hi Louis,

The steroids can reduce inflammation in the liver, which can bring down those enzyme levels. Aside from that, it's typical to avoid alcohol and salt, and (more as a long-term strategy) eat a low-protein, high-carb diet.

Good luck in getting those numbers to acceptable levels very quickly.

JimC
Forum moderator

There isn't any specific intervention here, and the less added, the better. It's not likely that dexamethasone will make things worse, but there's no food or supplement that should be pursued to lower liver tests -- it's at least as likely if not more so that some well-intended supplement will make things worse vs. make things better.

Good luck.

-Dr. West

Louis

Your wife's story is an amazing one. I wish her well on the new trial. Please keep us posted and good luck!

Bob

That's wonderful news, Louis! Good luck. It's a very promising drug in this setting!

-Dr. West

Hi louisb, I'm so sorry your wife has progression.

When lung cancer spreads to other parts of the body the tissue is still composed of lung cells and with the exception of the brain, responds the same whether in the lung or liver. Sometimes progression happens in one tumor but not another such as when there's progression in the liver but not the lung. This suggests the liver tumor has acquired a resistant mutation to the drug. So there's not one therapy that would be better for a liver met than a lung tumor. All of the chemo agents you've mentioned would be good choices especially if it was the platinum drug that caused Lynda's reaction. Everyone is different but alimta has the reputation of being less toxic than others and taxanes have a bad rep for causing neuropathy. Abraxane may be another option.

Since the immunotherapies aren't approved for lung cancer no one has experience clinically and all the data aren't in for our faculty to make a statement on one vs another.

As far as mutation testing there's a lot going on in the way of testing for mutations whether they're treatable or not. This is more of a social media advancement of finding more people with mutations rather than having a treatment to offer those with those mutations. Someone else is likely to have a better answer.

I hope Lynda does well with her next treatment for a long long time,
Janine

Hi louisb,

I'd agree with what Janine has said. There isn't one type of systemic treatment (whether chemo or targeted therapy) which has provided strong evidence that it is more effective against brain metastases. And any of the options you mention can be effective against tumors in both the lung and liver.

Certainly a new biopsy could be performed, but whether the information uncovered would lead to a specialized choice of treatment is not at all clear. It's becoming clear that many patients' cancers consist of more than one type, so that targeting one mutation that has been found may not be effective against the rest of the cancer cells which do not harbor that same mutation.

Good luck with whichever treatment choice is made.

JimC
Forum moderator

louisb,

None of the chemo drugs is any better specifically against the cancer in any particular part of the body such as the liver.

JimC
Forum moderator

Louis,

I'm afraid you're asking questions that can't be answered. None of the treatments that you are asking about has been studied enough to say what to expect. The various immunotherapy agents have all shown activity in a minority of people with previously treated NSCLC, but there is no way to compare the efficacy of one vs. another, nor against the long list of chemo agents that are potential options but haven't been studied enough to say how effective they might be in previously treated patients.

-Dr. West