Are you currently (or have you been) in a Clinical Trial?

Oh Nicole, that liver resection does not sound fun. I hope you start feeling better soon and that Enhertu is both kind and powerful.

All of you STAGE IV ladies are heroes in my eyes as I read about your personal experiences with this Bitch of a Disease. I am only now going into this basically new since I was naive enough to believe I actually had beat this 13 yeas ago StageIIIA. NED all these years and then getting that call from my ONC to getin for scans immediately…..Boom !!!…STAGE IV Mets to Ribs left and. right, Spine, T & L. Multiple mets throughout,including Sacrum left & right, and Ilia😲… feeling SHOCK, FEAR, sudden Determination to be Optimistic and even Cheerful and act as if nothing has changed…All to encourage my children and other family & Friends. I don’t want them to ink into a negative fear of losing me any day.. Dear nicolerod, my prayers are with you as you face yet another fight with this Bitch of a disease.😞💗

Anything exciting coming out of ASCO? Looks like there was something meaningful in regards to Piqray, but Cure-ious I defer to your knowledge :)

Hi all. I just started a clinical trial on June 1st. The drug is called RLY-2608. It is a drug that targets the PIK3 mutation. They are hoping it will be less harsh on patients than Piqray, and also of course be effective. It is a phase 1 trial, so I know I am getting the drug. From what I’ve read, I am getting a much higher dosage than patients in the early part of the trial. I didn’t even last 6 months on ibrance/fulvestrant so I’m really hoping this drug can at least stabilize things. My bone Mets responded to ibrance but liver Mets kept increasing.

Here is what was presented at ASCO regarding the BLU-222 CDK2 inhibitor trial I was on. On the poster, I’m patient 4 -the only partial response patient. When they measured pRb%, I was greater than 12 hours since my last dose because I couldn’t eat before my biopsy and needed to eat to take my pills. They commented that my pRb% may have been better than actually shown. I’m CCNE1 amplified. It looks like they are going to see if they get better efficacy combining this drug with others. And yes, that’s my liver on the poster. Lol. How did they leave off that I suffered from horrendous diarrhea?
https://www.blueprintmedicines.com/wp-content/uploads/2023/06/Blueprint-Medicines-ASCO-2023-BLU-222-VELA-Monotherapy-Dose-Escalation-Poster.pdf

https://scrip.pharmaintelligence.informa.com/SC148486/ASCO-2023--Pfizer-Pushes-Forward-In-Drug-Resistant-Breast-Cancer

Thanks rk2020 for the two links. It's interesting to see the update for your trial, but a shame BLU-222 didn't work for you longer. It was also good to read all the Pfizer is doing with its new inhibitors.

They just added fulvestrant shots to my combo of CDK2 & CDK4 inhibitors - hopefully third time will work as it did for tries #1 and #2. My side effects have stabilized to manageable now following the reduction in the CDK4 dose. I'll see if I can track down more info on the ASCO presentations re the drugs, I lost sight that it was on (likely because I left twitter).

My next trial scan is in 2 weeks.

@newgardener - I’m thrilled that you are doing well on the Pfizer trial! I just checked in this morning with someone else I know on the Pfizer trial. Unfortunately, she had a mixed response after 2 months so she dropped out.

I had an 8 week CT last Thursday for my AC699 PROTAC trial but don’t yet have the results. 😟My doctor is at ASCO and hasn’t pushed the results to my portal yet. 😩 My bone scan is done at a different facility so I have those results. Bone mets stable except for something possibly lurking in my left jaw. My chin and left jaw have been numb since May 7. Brain MRI was clear except for 2 low intensity skull lesions. Bone scan said left mandible suspicious for additional osseous metastasis. I don’t know what to think but I cancelled my Zometa infusion that I was supposed to get today. Ive been on it quarterly for 3 years and was thinking it’s time to stop but my doctor wanted me to stay on it. Nonetheless, I’m going to stop until I can get a better handle on what’s going on with my jaw. My body. My choice. Due to ASCO, I guess I won’t get my CT result until tomorrow. I’ve got concerns over spleen/pancreas area as well as my liver. I’m really not good at waiting. Good or bad…I want to know.

Dear all, I think these results will pave a quick pathway for approval of PDXd (first, most probably in the US): https://www.onclive.com/view/her3-dxd-elicits-responses-and-safety-in-heavily-pretreated-er-breast-cancer-and-tnbc

AC699 PROTAC estrogen receptor degrader 8 week scan results:

Bones stable except area of concern in my jaw. Liver lesions growing by leaps and bounds. Trial over for me. Not unexpected but disappointing nonetheless.

Dear rk2020, sorry for the news. But then let's think that maybe this dang progression has opened doors for something else. Also, fast growing suckers, if hit right, suffer quickly. So now we could think of targeting trop2, her2low and her3 (you must have expression to make PDXd useful - but quite many cells have it, we see it in clinical trial)? Have you discussed anything with your clinical investigators or your MO, what options there could be? Hugs,

Saulius

Can anyone please explain to me in EASY to UNDERSTAND terms the Difference between CAR-T and TIL? I know what TILs do or should I say how it works..but I am not clear about the CAR T…. should be looking into CART instead of this TIL???

Dear Nicole, the difference is that these two are different strategies: TILs - lymphocytes taken from your tumor (means they are fighting the tumor and recognize it), multiplied in the dishes/labs and brought back to you in big numbers, CAR-T - lymphocytes taken from your blood, re-engineered in the lab for specific antigens, brought back to you, multiplied inside of you with growth factor hormones. TILs are much more specific, probably fighting more expressions/antigens and reaching solid tumor better, as of today. CAR-Ts usually are re-engineered for one specific mutation and work well in some blood and lymph cancers where delivery is a minor issue, and where cancers have that very specific mutation. CAR-Ts stay in the body (blood, lymph) for many years "patrolling" it, TILs don't (please correct me if I am wrong). There are many studies for CAR-Ts for solid tumors but I'd say they are not very successful yet, and there's no data that would help us to compare TILs-fST vs CAR-Ts-fST:/ That, for sure, sucks…

Saulius

rk2020- I'm sorry your liver is going crazy and happy that the protac worked for your bones. it sounds like protac might work better in combination with something that works in the liver. bones often are indolent and don't work with the same drugs that help the liver so much.

Enhertu would seem like a good choice- IV every 3 weeks, 50% lose hair, in Destiny 04 worked in ~50% of heavily pre-treated (average 7 prior therapies) for PFS of 10.5 months. No data for bone only. they are doing a study on Her 2 zero as well. the first cycle is dicey, but, gets better, it is not working robustly for me (bone only) but, keeping me stable- I think I will make the 10 months- but not much more. They are using tons of it where I am.

Have you ever been Her 2 low?

rk2020, I am very sorry to hear about the progression. You are in my thoughts and prayers. The Enhertu sounds like a good next option.