Disconcerting news today

Mark,

Sorry I don't have any knowledge of this type condition.  Hopefully others will chime in soon.  Just wanted to let you know how sorry I am about the news and I'll be praying for you.  Best of luck with your upcoming decision.  Sounds like you have some pretty good options.

Brian

Mark,

Sorry I don't have any knowledge of this type condition.  Hopefully others will chime in soon.  Just wanted to let you know how sorry I am about the news and I'll be praying for you.  Best of luck with your upcoming decision.  Sounds like you have some pretty good options.

Brian

Mark,

Sorry I don't have any knowledge of this type condition.  Hopefully others will chime in soon.  Just wanted to let you know how sorry I am about the news and I'll be praying for you.  Best of luck with your upcoming decision.  Sounds like you have some pretty good options.

Brian

I am very sorry about the new, but I agree with Brian – it sounds like you have some excellent options there. Please keep posting about your progress.

I am very sorry about the new, but I agree with Brian – it sounds like you have some excellent options there. Please keep posting about your progress.

I am very sorry about the new, but I agree with Brian – it sounds like you have some excellent options there. Please keep posting about your progress.

Sorry Mark,

I know this is not at all what you were hoping for.  I am not a melanoma/bone expert, but am pretty well read on the data and don't know of anything more particular or different in the approach to that as opposed to other melanoma lesions other than perhaps a greater use of radiation like the others have said.  I agree also that you have some options with maybe BRAF or the BRAF/MEK combo at least until anti-PD1 comes on the market and perhaps you could try that then if need be.  There are also trials with antiPDL, the new ADC drug (I know they are still taking occasional patients in Nashville, though I don't know your location or all the trial requirements).  Some places including Moffitt are doing trials with Rose Bengal (PV-10) but you must have a lesion superficial enough to inject and I'm not sure it sounds as though you do.  One other ray of light if your onc does recommend radiation (and I'm not saying they should or shouldn't)…but if they do…there is more and more data showing the benefits of the ipi/radiation combo…even when the patient didn't respond so well to ipi in the first place.  I recently posted some articles talking about that on my blog.

Wishing you my best. Hang in there. Celeste

Sorry Mark,

I know this is not at all what you were hoping for.  I am not a melanoma/bone expert, but am pretty well read on the data and don't know of anything more particular or different in the approach to that as opposed to other melanoma lesions other than perhaps a greater use of radiation like the others have said.  I agree also that you have some options with maybe BRAF or the BRAF/MEK combo at least until anti-PD1 comes on the market and perhaps you could try that then if need be.  There are also trials with antiPDL, the new ADC drug (I know they are still taking occasional patients in Nashville, though I don't know your location or all the trial requirements).  Some places including Moffitt are doing trials with Rose Bengal (PV-10) but you must have a lesion superficial enough to inject and I'm not sure it sounds as though you do.  One other ray of light if your onc does recommend radiation (and I'm not saying they should or shouldn't)…but if they do…there is more and more data showing the benefits of the ipi/radiation combo…even when the patient didn't respond so well to ipi in the first place.  I recently posted some articles talking about that on my blog.

Wishing you my best. Hang in there. Celeste

Sorry Mark,

I know this is not at all what you were hoping for.  I am not a melanoma/bone expert, but am pretty well read on the data and don't know of anything more particular or different in the approach to that as opposed to other melanoma lesions other than perhaps a greater use of radiation like the others have said.  I agree also that you have some options with maybe BRAF or the BRAF/MEK combo at least until anti-PD1 comes on the market and perhaps you could try that then if need be.  There are also trials with antiPDL, the new ADC drug (I know they are still taking occasional patients in Nashville, though I don't know your location or all the trial requirements).  Some places including Moffitt are doing trials with Rose Bengal (PV-10) but you must have a lesion superficial enough to inject and I'm not sure it sounds as though you do.  One other ray of light if your onc does recommend radiation (and I'm not saying they should or shouldn't)…but if they do…there is more and more data showing the benefits of the ipi/radiation combo…even when the patient didn't respond so well to ipi in the first place.  I recently posted some articles talking about that on my blog.

Wishing you my best. Hang in there. Celeste

I'm in the same situation. So far all my mel is in/on my bones. So far the only thing that worked some was radiation. It was targetted pallative that reduced that area 20%. 8 weeks of max zelboraf did nothing to shrink any mel. For that everything grew except the radiated area. I get my 4th/final ipi dose monday so won't know for quite awhile how it has done.

I'm in the same situation. So far all my mel is in/on my bones. So far the only thing that worked some was radiation. It was targetted pallative that reduced that area 20%. 8 weeks of max zelboraf did nothing to shrink any mel. For that everything grew except the radiated area. I get my 4th/final ipi dose monday so won't know for quite awhile how it has done.

I'm in the same situation. So far all my mel is in/on my bones. So far the only thing that worked some was radiation. It was targetted pallative that reduced that area 20%. 8 weeks of max zelboraf did nothing to shrink any mel. For that everything grew except the radiated area. I get my 4th/final ipi dose monday so won't know for quite awhile how it has done.

If you are in good shape, HD IL-2 is a valid treatment to try if one has a very experienced Oncologist and staff with its administration/side effects.. While only providing a positive response for around 20% of patients, it has provided what is being referred to as a CURE to about 5% of recipients. It is a tough, but do-able treatment with a quick recovery time from each treatment week. (I received 49 bags and was a partial responder for 20 months.) Others have bee free from Melanoma fro over 20 years from IL-2 administration. For some people Ipi has less short term side effects, for others,Ipi has long/longer lasting negative side effects.

If you are in good shape, HD IL-2 is a valid treatment to try if one has a very experienced Oncologist and staff with its administration/side effects.. While only providing a positive response for around 20% of patients, it has provided what is being referred to as a CURE to about 5% of recipients. It is a tough, but do-able treatment with a quick recovery time from each treatment week. (I received 49 bags and was a partial responder for 20 months.) Others have bee free from Melanoma fro over 20 years from IL-2 administration. For some people Ipi has less short term side effects, for others,Ipi has long/longer lasting negative side effects.

If you are in good shape, HD IL-2 is a valid treatment to try if one has a very experienced Oncologist and staff with its administration/side effects.. While only providing a positive response for around 20% of patients, it has provided what is being referred to as a CURE to about 5% of recipients. It is a tough, but do-able treatment with a quick recovery time from each treatment week. (I received 49 bags and was a partial responder for 20 months.) Others have bee free from Melanoma fro over 20 years from IL-2 administration. For some people Ipi has less short term side effects, for others,Ipi has long/longer lasting negative side effects.