NPfisherman1 year ago

There was a study done some time ago showing that Gleason 9 and 10 did not fare as well with intermittent therapy, but the treatment paradigm is rapidly changing... The likelihood your T will come back decreases when you go beyond 24 months of ADT.

Currently, I am doing intermittent using Eligard and abiraterone with SBRT to oligometastatic lesions when they arise. I am still on treatment now.

The first round, I did 22 months on treatment, and about month 16 of vacation, I had the initial indication of a BCR. I waited to do Pylarify at about 0.8 and found one lesion. Gave myself Eligard and timed for a testosterone flare to get my SBRT. We will see how it goes with round 2, since I may be starting vacation in a few months if things continue to go well. My first vacation lasted 22 months...same as treatment... This time, my treatment is 1 year...

The Pylarify scan you did while "undetectable" means nothing. You need a PSA of about 0.5 or greater to hope for an accurate Pylarify scan.

If you do go on vacation, you may want to watch hormone levels. Some take tamoxifen or exemastane for E levels. Dutasteride or finasteride for DHT and T. Mucuna L dopa gtts or mucuna pruriens for prolactin levels.

Hope some of my ramblings are helpful to you... Good luck on your path...

Don Pescado

Bhraen2 in reply to NPfisherman1 year ago

Thank you Don. Very helpful information. It seems my MO is hoping for the same success with my treatment break as you’ve had. Glad to hear from someone who has gone through it and had good results. I appreciate you giving me a heads up about the hormone levels and how to keep them in check. I wasn’t thinking about that and now realize how important it would be.

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Hidden1 year ago

25-30% chance of turning into neuroendocrine? REally? What says that? Thanks

Bhraen2 in reply to Hidden1 year ago

It’s what I was told by my MO when I questioned him about it. Maybe has to do with my Gleason 9 pathology and ATM mutation.

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Papillon21 year ago

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pjoshea131 year ago

You asked about BAT. With Samuel Denmeade's BAT, of course, you would be back on ADT, with a shot of testosterone cypionate every 28 days. T would oscillate from supraphysiological to near-castrate. Although men on BAT continue on ADT, there is no meaningful period of castrate T.

An alternative scenario is that you remain on ADT vacation for three months, say, but with restored testosterone [T] of, say, 1,000 ng/dL. A variation would be to used double the T-cypionate dose, to get T up to 2,000 ng/dL, in the hope of inducing double-strand breaks.

During the vacation, the PSA might rise (as it might with Denmeade's BAT). This can be stressful. Hopefully, you would get a real vacation with 3 months of high-normal or supra-high T. & perhaps the vacation might be extended.

You can return to ADT at any time. After 3 months of ADT it might be possible to repeat the vacation.

I view the purpose of T here is to reverse adaptations and turn back the clock. However, after 2 years of Lupron & Zytiga, who knows what adaptations have occurred? For example, the androgen receptor splice variant AR-V7 that lacks the androgen-binding domain.

I am not a doctor & have no idea as to how someone in your situation might respond to the scenario, so I can't recommend it. I hope others will respond and point out the risks.

Best, -Patrick

Bhraen2 in reply to pjoshea131 year ago

Thank you Patrick. I looked up some of your old posts, the one about the transformer trial was very helpful.

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Bhraen21 year ago

Thank you again. In the alternative situation of no ADT and a double cypionate injection, how often would the injection be repeated? And yes the purpose would be to set back the clock and reverse adaptations