dads metastatic melanoma treatment options

I've had IL-2 and ipilimumab (Yervoy), but not PD-1, but given the choice today without any other information or eligibility requirements (like a biomarker test that says that ipilimumab would be better for me specifically), I think PD-1 would have to be my first choice — simply, in the ongoing trials, it has demonstrated a higher response rate with fewer side effects than ipilimumab.  

However, it is widely believed that the approval of Merck's PD-1 (pembrolizumab) will, at least initially, come with a requirement that a patient first try and fail ipilimumab, in other words, the approval won't be as a first-line therapy for melanoma.  The early access programs (EAPs) for both Merck's and BMS's PD-1 therapies are structured the same way (BRAF-positive patients must have also tried and failed a BRAF agent, but that doesn't apply to your father).  A few things to note, though:  (1) I have heard from more than one medical professional "in the know" that it isn't 100% guaranteed that the approval will come with this ipilimumab-first requirement, (2) the approval for pembrolizumab may be coming sooner than late October, as soon as the next few weeks, according to an article today on Reuters (http://www.reuters.com/article/2014/08/25/us-merck-cancer-fda-idUSKBN0GP0VU20140825) — granted, that puts us in mid-September, but it is a little sooner, and (3) if the ipilimumab-first requirement is initially put in place, the expectation is that it would probably be "lifted" after perhaps six months or so, after the final Phase III trial results are submitted and reviewed by the FDA.

The challenge is that there are a lot of "what-ifs" that may take up to two months before there are answers, and no guarantee what those answers may be.  Within two months (9 weeks from first dose to last dose), your father could complete a full four-dose course of ipilimumab.  As noted in your post, clinical trials are also an option — the EAPs, as I mentioned above wouldn't be an option because of the ipilimumab-first requirement.  You could seek out a trial for PD-1 and there are trials combining BMS's PD-1 (nivolumab) with ipilimumab (also a BMS product).  I think you may have mentioned in an earlier post that your father's primary residence is out-of-country — I don't know if that factors into insurance, cost, or anything, so I'm just setting that aside for this conversation.  

Did Drs. O'Day or Wong make any recommendations (or strong suggestions), or simply explain the options?  Also, what are your plans for the needle biopsy?  Will you be proceeding with that and if so, when?  Given the size (1-cm is relatively small), I'm guessing that he's not having any symptoms associated with the presence of the two of them, but that's just a guess.  And they could be very slow-growing and stay stable in size well past the time that the FDA approves Merck's PD-1, or they might not — another "what-if".

So, long story short, back to your original question and factoring in the timing and approval requirements for PD-1, if it were me today, I'd probably either start ipilimumab sooner-rather-than-later, or find a trial for nivolumab plus ipilimumab.  That, of course, is my opinion, I hope many others weigh in here, too, with their thoughts.  For what it's worth, you've taken a sound approach and sought out experts in the field and are doing all the right things — remember that there won't be a perfect decision because of the unanswerable questions that are still out there.  Wishing you and your father the best!

Joe

I've had IL-2 and ipilimumab (Yervoy), but not PD-1, but given the choice today without any other information or eligibility requirements (like a biomarker test that says that ipilimumab would be better for me specifically), I think PD-1 would have to be my first choice — simply, in the ongoing trials, it has demonstrated a higher response rate with fewer side effects than ipilimumab.  

However, it is widely believed that the approval of Merck's PD-1 (pembrolizumab) will, at least initially, come with a requirement that a patient first try and fail ipilimumab, in other words, the approval won't be as a first-line therapy for melanoma.  The early access programs (EAPs) for both Merck's and BMS's PD-1 therapies are structured the same way (BRAF-positive patients must have also tried and failed a BRAF agent, but that doesn't apply to your father).  A few things to note, though:  (1) I have heard from more than one medical professional "in the know" that it isn't 100% guaranteed that the approval will come with this ipilimumab-first requirement, (2) the approval for pembrolizumab may be coming sooner than late October, as soon as the next few weeks, according to an article today on Reuters (http://www.reuters.com/article/2014/08/25/us-merck-cancer-fda-idUSKBN0GP0VU20140825) — granted, that puts us in mid-September, but it is a little sooner, and (3) if the ipilimumab-first requirement is initially put in place, the expectation is that it would probably be "lifted" after perhaps six months or so, after the final Phase III trial results are submitted and reviewed by the FDA.

The challenge is that there are a lot of "what-ifs" that may take up to two months before there are answers, and no guarantee what those answers may be.  Within two months (9 weeks from first dose to last dose), your father could complete a full four-dose course of ipilimumab.  As noted in your post, clinical trials are also an option — the EAPs, as I mentioned above wouldn't be an option because of the ipilimumab-first requirement.  You could seek out a trial for PD-1 and there are trials combining BMS's PD-1 (nivolumab) with ipilimumab (also a BMS product).  I think you may have mentioned in an earlier post that your father's primary residence is out-of-country — I don't know if that factors into insurance, cost, or anything, so I'm just setting that aside for this conversation.  

Did Drs. O'Day or Wong make any recommendations (or strong suggestions), or simply explain the options?  Also, what are your plans for the needle biopsy?  Will you be proceeding with that and if so, when?  Given the size (1-cm is relatively small), I'm guessing that he's not having any symptoms associated with the presence of the two of them, but that's just a guess.  And they could be very slow-growing and stay stable in size well past the time that the FDA approves Merck's PD-1, or they might not — another "what-if".

So, long story short, back to your original question and factoring in the timing and approval requirements for PD-1, if it were me today, I'd probably either start ipilimumab sooner-rather-than-later, or find a trial for nivolumab plus ipilimumab.  That, of course, is my opinion, I hope many others weigh in here, too, with their thoughts.  For what it's worth, you've taken a sound approach and sought out experts in the field and are doing all the right things — remember that there won't be a perfect decision because of the unanswerable questions that are still out there.  Wishing you and your father the best!

Joe

I've had IL-2 and ipilimumab (Yervoy), but not PD-1, but given the choice today without any other information or eligibility requirements (like a biomarker test that says that ipilimumab would be better for me specifically), I think PD-1 would have to be my first choice — simply, in the ongoing trials, it has demonstrated a higher response rate with fewer side effects than ipilimumab.  

However, it is widely believed that the approval of Merck's PD-1 (pembrolizumab) will, at least initially, come with a requirement that a patient first try and fail ipilimumab, in other words, the approval won't be as a first-line therapy for melanoma.  The early access programs (EAPs) for both Merck's and BMS's PD-1 therapies are structured the same way (BRAF-positive patients must have also tried and failed a BRAF agent, but that doesn't apply to your father).  A few things to note, though:  (1) I have heard from more than one medical professional "in the know" that it isn't 100% guaranteed that the approval will come with this ipilimumab-first requirement, (2) the approval for pembrolizumab may be coming sooner than late October, as soon as the next few weeks, according to an article today on Reuters (http://www.reuters.com/article/2014/08/25/us-merck-cancer-fda-idUSKBN0GP0VU20140825) — granted, that puts us in mid-September, but it is a little sooner, and (3) if the ipilimumab-first requirement is initially put in place, the expectation is that it would probably be "lifted" after perhaps six months or so, after the final Phase III trial results are submitted and reviewed by the FDA.

The challenge is that there are a lot of "what-ifs" that may take up to two months before there are answers, and no guarantee what those answers may be.  Within two months (9 weeks from first dose to last dose), your father could complete a full four-dose course of ipilimumab.  As noted in your post, clinical trials are also an option — the EAPs, as I mentioned above wouldn't be an option because of the ipilimumab-first requirement.  You could seek out a trial for PD-1 and there are trials combining BMS's PD-1 (nivolumab) with ipilimumab (also a BMS product).  I think you may have mentioned in an earlier post that your father's primary residence is out-of-country — I don't know if that factors into insurance, cost, or anything, so I'm just setting that aside for this conversation.  

Did Drs. O'Day or Wong make any recommendations (or strong suggestions), or simply explain the options?  Also, what are your plans for the needle biopsy?  Will you be proceeding with that and if so, when?  Given the size (1-cm is relatively small), I'm guessing that he's not having any symptoms associated with the presence of the two of them, but that's just a guess.  And they could be very slow-growing and stay stable in size well past the time that the FDA approves Merck's PD-1, or they might not — another "what-if".

So, long story short, back to your original question and factoring in the timing and approval requirements for PD-1, if it were me today, I'd probably either start ipilimumab sooner-rather-than-later, or find a trial for nivolumab plus ipilimumab.  That, of course, is my opinion, I hope many others weigh in here, too, with their thoughts.  For what it's worth, you've taken a sound approach and sought out experts in the field and are doing all the right things — remember that there won't be a perfect decision because of the unanswerable questions that are still out there.  Wishing you and your father the best!

Joe

If it were me, I would wait for PD1 to be approved by the FDA because the cure rate is higher than other treatments.

The ONLY problem with waiting is that a patient might be required by the FDA to have "failed" yervoy first. Even though the doctor culd prescribe PD1, your insurance might not pay for the drug unless the patient fails Yervoy first.

What did Dr.O'day & Dr.Wong tell you about first having to FAIL Yervoy f beforeyou can get PD1 once it is approved by the FDA?

If it were me, I would wait for PD1 to be approved by the FDA because the cure rate is higher than other treatments.

The ONLY problem with waiting is that a patient might be required by the FDA to have "failed" yervoy first. Even though the doctor culd prescribe PD1, your insurance might not pay for the drug unless the patient fails Yervoy first.

What did Dr.O'day & Dr.Wong tell you about first having to FAIL Yervoy f beforeyou can get PD1 once it is approved by the FDA?

If it were me, I would wait for PD1 to be approved by the FDA because the cure rate is higher than other treatments.

The ONLY problem with waiting is that a patient might be required by the FDA to have "failed" yervoy first. Even though the doctor culd prescribe PD1, your insurance might not pay for the drug unless the patient fails Yervoy first.

What did Dr.O'day & Dr.Wong tell you about first having to FAIL Yervoy f beforeyou can get PD1 once it is approved by the FDA?

Just a couple of thoughts on the options you now face. The % on the PD-1 alone are ranging between 30-40% not 65%. The survival data on the combination of Ipi and PD-1 (Nivolumab) together is coming back really strong with 1 year survival #'s in the 80% range and 2 year survival in the 70% range. Down side the risk of drug related reaction are also higher with the combination group. If the lung nodules are not aggressive the waiting for approval of PD-1 might be a good way to go. Or look for expanded access to clinical trials of the combination Ipi and nivolumab. I waited from July of last year until Jan of 2014 to get into the Bristol Myer squibb trial of Ipi and Nivolumab and happy today that I did. I hope things go slow and many options are available. Ed

Just a couple of thoughts on the options you now face. The % on the PD-1 alone are ranging between 30-40% not 65%. The survival data on the combination of Ipi and PD-1 (Nivolumab) together is coming back really strong with 1 year survival #'s in the 80% range and 2 year survival in the 70% range. Down side the risk of drug related reaction are also higher with the combination group. If the lung nodules are not aggressive the waiting for approval of PD-1 might be a good way to go. Or look for expanded access to clinical trials of the combination Ipi and nivolumab. I waited from July of last year until Jan of 2014 to get into the Bristol Myer squibb trial of Ipi and Nivolumab and happy today that I did. I hope things go slow and many options are available. Ed

Just a couple of thoughts on the options you now face. The % on the PD-1 alone are ranging between 30-40% not 65%. The survival data on the combination of Ipi and PD-1 (Nivolumab) together is coming back really strong with 1 year survival #'s in the 80% range and 2 year survival in the 70% range. Down side the risk of drug related reaction are also higher with the combination group. If the lung nodules are not aggressive the waiting for approval of PD-1 might be a good way to go. Or look for expanded access to clinical trials of the combination Ipi and nivolumab. I waited from July of last year until Jan of 2014 to get into the Bristol Myer squibb trial of Ipi and Nivolumab and happy today that I did. I hope things go slow and many options are available. Ed

My quick 2 cents.  The treatments with proven "home run" potential (cure) are IL-2 (low percentage as noted), TIL and ipi.  If I were starting fresh at this point in time, I'd aim for the ipi/nivolumab combo EAP or TIL.  Either path has potential for rough side effects–with a big payoff.  Just my opinion.

My quick 2 cents.  The treatments with proven "home run" potential (cure) are IL-2 (low percentage as noted), TIL and ipi.  If I were starting fresh at this point in time, I'd aim for the ipi/nivolumab combo EAP or TIL.  Either path has potential for rough side effects–with a big payoff.  Just my opinion.

My quick 2 cents.  The treatments with proven "home run" potential (cure) are IL-2 (low percentage as noted), TIL and ipi.  If I were starting fresh at this point in time, I'd aim for the ipi/nivolumab combo EAP or TIL.  Either path has potential for rough side effects–with a big payoff.  Just my opinion.

Hi Liam,

I'm going to go out on a limb here and share with you some melanoma treatments I have been using which are not standard of care, (SOC).  I do have an oncologist and along the 3 year path have had surgeries ,(Stage 3 met/mel,) however I am sure that I am doing so well because of dietary changes and medicines which are better known in Europe than in US.  Some things to look into.  Helixor Mistletoe Pini (from Pine tree.)  I've heard that Mistletoe is the most prescribed cancer medicine in the world. M.D. or N.D. perscription and guidance needed and   "AVemar"  a nutritional powder, much research on Melanoma,   Eat whole food.  Remove processed food. Stop eating sugar.  Some fruit is OK. Eat only good oils, olive, coconut, raw flax.  The Budwig diet is a whole protocol… I eat their primary mix (3T. FO/CC Flax Oil , 6T cottage cheese  emulsified and 2T ground flax,) once per day.  Fermented vegetables (saurekraut,) and Beet Kvass. There are many supplements as well.  If interested I'll share it complete .  I also have done 3 rounds of whole body and regional hyperthermia in B.C. Canada.    I am BRAF pos, have been offered interlukin, IL-2 and Zelboraf.  I have opted for surgery and hyperthermia.  I have had PET/CT every 6 months and MRI as necessary.  Am at this moment considering steriotactic radiotherapy for 1 tumor.  I've found that being open to all options has worked best for me.  There are Naturopathic doctors who specialize in cancer treatment, suffix of FABNO is used.  .  They and anthoposophical doctors will know about Mistletoe. My strategy has been to support my immune system and to use SOC treatments to debulk (remove tumor mass,) as necessary.  The pending PD-1 drugs sound promising.   Wishing you and your dad all the best on this journey.  You can live with melanoma.   Aloha, Ann

Hi Liam,

I'm going to go out on a limb here and share with you some melanoma treatments I have been using which are not standard of care, (SOC).  I do have an oncologist and along the 3 year path have had surgeries ,(Stage 3 met/mel,) however I am sure that I am doing so well because of dietary changes and medicines which are better known in Europe than in US.  Some things to look into.  Helixor Mistletoe Pini (from Pine tree.)  I've heard that Mistletoe is the most prescribed cancer medicine in the world. M.D. or N.D. perscription and guidance needed and   "AVemar"  a nutritional powder, much research on Melanoma,   Eat whole food.  Remove processed food. Stop eating sugar.  Some fruit is OK. Eat only good oils, olive, coconut, raw flax.  The Budwig diet is a whole protocol… I eat their primary mix (3T. FO/CC Flax Oil , 6T cottage cheese  emulsified and 2T ground flax,) once per day.  Fermented vegetables (saurekraut,) and Beet Kvass. There are many supplements as well.  If interested I'll share it complete .  I also have done 3 rounds of whole body and regional hyperthermia in B.C. Canada.    I am BRAF pos, have been offered interlukin, IL-2 and Zelboraf.  I have opted for surgery and hyperthermia.  I have had PET/CT every 6 months and MRI as necessary.  Am at this moment considering steriotactic radiotherapy for 1 tumor.  I've found that being open to all options has worked best for me.  There are Naturopathic doctors who specialize in cancer treatment, suffix of FABNO is used.  .  They and anthoposophical doctors will know about Mistletoe. My strategy has been to support my immune system and to use SOC treatments to debulk (remove tumor mass,) as necessary.  The pending PD-1 drugs sound promising.   Wishing you and your dad all the best on this journey.  You can live with melanoma.   Aloha, Ann

Hi Liam,

I'm going to go out on a limb here and share with you some melanoma treatments I have been using which are not standard of care, (SOC).  I do have an oncologist and along the 3 year path have had surgeries ,(Stage 3 met/mel,) however I am sure that I am doing so well because of dietary changes and medicines which are better known in Europe than in US.  Some things to look into.  Helixor Mistletoe Pini (from Pine tree.)  I've heard that Mistletoe is the most prescribed cancer medicine in the world. M.D. or N.D. perscription and guidance needed and   "AVemar"  a nutritional powder, much research on Melanoma,   Eat whole food.  Remove processed food. Stop eating sugar.  Some fruit is OK. Eat only good oils, olive, coconut, raw flax.  The Budwig diet is a whole protocol… I eat their primary mix (3T. FO/CC Flax Oil , 6T cottage cheese  emulsified and 2T ground flax,) once per day.  Fermented vegetables (saurekraut,) and Beet Kvass. There are many supplements as well.  If interested I'll share it complete .  I also have done 3 rounds of whole body and regional hyperthermia in B.C. Canada.    I am BRAF pos, have been offered interlukin, IL-2 and Zelboraf.  I have opted for surgery and hyperthermia.  I have had PET/CT every 6 months and MRI as necessary.  Am at this moment considering steriotactic radiotherapy for 1 tumor.  I've found that being open to all options has worked best for me.  There are Naturopathic doctors who specialize in cancer treatment, suffix of FABNO is used.  .  They and anthoposophical doctors will know about Mistletoe. My strategy has been to support my immune system and to use SOC treatments to debulk (remove tumor mass,) as necessary.  The pending PD-1 drugs sound promising.   Wishing you and your dad all the best on this journey.  You can live with melanoma.   Aloha, Ann