New here. My story. : In late November... - Advanced Prostate...

Advanced Prostate Cancer

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New here. My story.

Skipper238 profile image
44 Replies

In late November 2021, I was diagnosed with advanced Prostate Cancer. My PCa is believed to have metastasized to three lymph nodes (lower neck, diaphragm and lower back). I say “believed” because the metastasis has not been confirmed. My Gleason scores were all 9’s and 10’s. My oncologist and Urologist feel like the odds are 90%+ that these enlarged lymph nodes shown in my PET scan are due to the PCa and are not Lymphoma. They are planning to wait to confirm after a couple of months of ADT and a future PET scan. My PSA was low, at 4.68.

I am taking Eligard (6 month dosage) and Bi. (50 mg tablet), and as a pre-diabetic am taking Metformin. I will supplement with daily calcium, magnesium and D3.

I am reading and learning and checking behind my doctors’ advice and information, which has been amazingly little. I understand they are busy with many patients, but I have been surprised at how committed they are to their 15 minute appointment time slots. Nevertheless, I am educating myself and also planning a second opinion on treatment plan via MD Anderson in Jacksonville, FL.

I wish everyone well with their treatments and results. 👍

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Skipper238
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Justfor_ profile image
Justfor_

When you say PET scan is it PSMA PET/CT or other?

Skipper238 profile image
Skipper238

Hello Just For__, Here are my PET scan summary notes.

(PET CT Skull to Thigh Initial) Reason For Exam: PET INITIAL STAGING LYMPHADENOPATHY

Read

HISTORY: PET INITIAL STAGING LYMPHADENOPATHY

PROCEDURE: PET CT Skull to Thigh Initial

COMPARISON: No comparison PET/CT. Comparison is made to CT of abdomen and pelvis dated

11/5/2021

CLINICAL HISTORY: Lymphadenopathy

TECHNICAL INFORMATION: Approximately 1 hour after IV administration of a 15 mCi dose of F18-

FDG, multiple scintigraphic images were obtained through the neck, chest, abdomen and pelvis

using a dedicated full-ring pet detector. Non-contrasted CT images and PET CT fusion images are

included for review.

FINDINGS: There is FDG avid lymphadenopathy above and below the diaphragm. Above the

diaphragm, there are 2 immediately adjacent markedly FDG avid left supraclavicular lymph nodes

measuring 2.7 x 1.5 cm in conglomerate, with maximum SUV of 19.7.

Below the diaphragm, there is FDG avid retroperitoneal and retrocrural lymphadenopathy. The

most FDG avid lymph node is an aortocaval lymph node (image 234) which measures 1.4 cm in short

axis, maximum SUV of 33.9. There is bilateral iliac lymphadenopathy.

There is increased FDG uptake in the prostate, with maximum SUV of 11.5. A 3 cm right adrenal

nodule measures fat attenuation compatible with an adenoma and demonstrates mild FDG uptake,

maximum SUV is 6.6.

There is a 2 mm right upper lobe nodule (image 134), too small to characterize with PET. There are

small bilateral fat-containing inguinal hernias. Diverticulosis without evidence of diverticulitis.

IMPRESSION:

1. Hypermetabolic left supraclavicular and retroperitoneal abdominal and pelvic lymphadenopathy

compatible with lymphoma.

2. Multiple foci of FDG avidity in the prostate. Recommend correlation with PSA and urologic

consult.

3. 3 cm right adrenal adenoma with mild FDG uptake.

Dictated: 11.23.2021 10:02 am Dictated By: Cail MD, Austin

Verified Date/Time: 11.23.2021 10:02 am Final Report Signed By: Cail MD, Austin

Magnus1964 profile image
Magnus1964

It's early, but it looks like you are on the right path.

Skipper238 profile image
Skipper238

Thank you, Magnus. That's reassuring, considering I'm only a handful of days into this thing, sort of, and as the joke goes, it could take me "weeks" to become an expert at PC!

I enjoy reading your posts.

Thanks.

Tall_Allen profile image
Tall_Allen

(1) Your FDG PET scan was a good choice because of your low PSA, and if the lymph nodes shrink after Lupron they are almost certainly due to prostate cancer. Before they disappear, you may want to ask for a biopsy of one of them. Histology and IHC analysis may reveal exactly what kind of prostate cancer it is, and, if enough tissue, a genomic analysis can provide further clues. For your next PET scan, you may want to have two of them - a repeat of the FDG scan to show shrinkage and a Pylarify PET scan to find if there are any PSMA-avid metastases.

(2) You should ask about SBRT to your prostate. In men with very few metastases, that has been shown to slow progression and improve survival:

prostatecancer.news/2018/09...

(3) Email the following link to your oncologist for discussion:

prostatecancer.news/2021/05...

You may need to ask for a double appointment next time to discuss all this.

maley2711 profile image
maley2711 in reply toTall_Allen

TA - Your article linked in ( 2 ) is really great, but don't see much there about SBRT application....is there the assumption that SBRT will be non-inferior to standard IMRT or hypofractionation?

Tall_Allen profile image
Tall_Allen in reply tomaley2711

Look again. They used SBRT in that study.

maley2711 profile image
maley2711 in reply toTall_Allen

I was reading your article

prostatecancer.news/2018/09...

All I see is this......

" were randomized to no radiation debulking or hypofractionated radiation, consisting of either:

55 Gy in 20 daily treatments, or

36 Gy in 6 weekly treatments (note: this bioequivalent dose is 15% higher) "

I also saw a brief mention of a new ongoing trial using SBRT....no results yet apparently.

Tall_Allen profile image
Tall_Allen in reply tomaley2711

36 Gy in 6 weekly treatments (note: this bioequivalent dose is 15% higher)

maley2711 profile image
maley2711 in reply toTall_Allen

Thanks TA,,,so it is the higher total dose that makes it SBRT.... # of sessions has nothing to do with SBRT?

Tall_Allen profile image
Tall_Allen in reply tomaley2711

You got that backwards.

Tall_Allen profile image
Tall_Allen

Why are you taking Calcium and those other chemicals? Did your blood work show a deficiency?

Skipper238 profile image
Skipper238 in reply toTall_Allen

Thanks for your replies, Tall_Allen. I will discuss all of the items you suggested with my Oncologist during my next appointment.

In terms of the calcium, etc., neither of my doctors have told me to take the supplement. I thought I needed to do it due to the ADT medicines Eligard and Bicalutamide. Do they not deplete calcium in the bones as they reduce testosterone in the body? Thx.

I've read many of your posts and appreciate your opinions and knowledge. Thank you for your time.

Tall_Allen profile image
Tall_Allen in reply toSkipper238

Taking extra calcium may encourage prostate cancer growth and may be harmful to the heart. It does nothing for your bones, if blood levels are normal. Similarly, Vitamin D does not improve bone health if levels are already normal. Resist the urge to flood your body with extra chemicals that you don't need. Just eat a healthy, varied diet - that will provide all the micronutrients you need and will support your microbiome. Exercise will do more for bone health than any of those.

Skipper238 profile image
Skipper238 in reply toTall_Allen

Thank you.

AlanMeyer profile image
AlanMeyer

Hello Skipper,

As Tall_Allen pointed out in a URL he sent you, the latest treatment recommendation for men with high risk, advanced prostate cancer is to to combine ADT with abiraterone, prednisone, and docetaxel. Allen quoted the trial report: "Radiographic progression-free survival increased by 2.5 years (from 2.0 to 4.5 yrs) with the addition of abiraterone to docetaxel" Two and a half years of extra life is a big deal! I don't understand why your oncologist is not following that, or at least the previous SOC that added either abiraterone+prednisone or docetaxel to ADT.

I understand that a doctor who makes appointments for every 15 minutes has to keep those appointments, but I'm not impressed by a doctor who only allocates 15 minutes to discuss serious life changing issues. I've had oncologists spend an hour with me.

I hope you get better treatment at M.D. Anderson. Please take the information Tall_Allen gave you to your appt. at Anderson.

Best of luck.

Alan

maley2711 profile image
maley2711 in reply toAlanMeyer

Agreed..... not impressed by what we've learned about that Doc? Standard at MD Anderson??

Skipper238 profile image
Skipper238 in reply tomaley2711

I don't think I was as clear as I could have been regarding this. My Oncologist and Urologist are from my local hospital system in Brunswick, Georgia, USA. I am in the processing of arranging a second opinion through MD Anderson in Jacksonville, FL, USA, which is 1.5 hours away from where I live. MD Anderson in Houston was my original choice for the second opinion, but they require an in-person visit. With COVID spreading and my life going full-speed, I'm just not going to get on a plane and fly to Houston, TX, unless my life depends on it. Hey, wait a minute. Maybe my life does depend on it! 😀

maley2711 profile image
maley2711 in reply toSkipper238

I'm confident, hopefully not proven wrong, that you will be happy with the expertise of the Anderson Docs. It is apparent that you are going to make a good decision, weighing QOL and long-term results. Unfortunately, we have no way to know whether a road we didn't choose would have resulted in more satisfactory outcome than what we experienced from the road we did choose....... will be interested to learn how much the Anderson Docs VOLUNTEER about the side effects of various treatment options. Everything is probabilities...I've learned that a probability that favored me isn't a predictor of my actual result!!!!! Sometimes that is good, sometimes NOT!! I often wonder if the men who just go with the flow of initial Doc advice do just as well as those who devote half of waking hours to researching this thing?

Skipper238 profile image
Skipper238 in reply tomaley2711

Thank you, Maley. I'm looking forward to meeting with the MD Anderson folks.

Skipper238 profile image
Skipper238 in reply toAlanMeyer

Thank you, Alan. I appreciate your post. I have read Tall's article, will review the study in detail and will discuss with the MD Anderson "second opinion" doctor(s) and my Oncologist, who is at my local hospital system in Georgia, U.S.A.

With that said (and I will ask for extra consideration on all of this, since my diagnosis was 8 days ago, and I am still processing my new reality and have a lot to learn, etc.), I noted a couple of things.

1. Early in the article, this point is made about about findings, I believe, from the Stampede trail.

"Serious toxicity (Grade 3 or greater) was also equal: 50% for docetaxel, 48% for abiraterone."

So, that is something I am trying to wrap my mind around related to quality of life. I have two children, ages 12 and 15, and although I want to be here for them as long as possible, I also want my quality of life to remain as high as possible for as long as possible. My feeling is that they will do better, long term, if they continue to see me as strong and viable and "normal" as possible for as long as possible. So, maybe that means that I should adopt this new SOC from the PEACE-1 study and introduce some downside to my quality of life early, so that I can have a longer and higher quality of life down the road. On the other hand, if I am able to ride ADT for 5 years and then introduce chemo and other, maybe that accomplishes my goal better. I am thinking about these things and hope people understand.

2. I am trying to understand how the conflict that "Tall" points out below applies to me. I believe my metastatic load to be "low", at the point.

Excerpt from "Tall's" article on PEACE study:

-------------------------------------------------------

"This controversy is reflected in the conflicting recommendations that constitute the standard of care.

The current NCCN guidelines state: "Docetaxel should not be offered to men with low volume metastatic prostate cancer, since this subgroup was not shown to have improved survival in either the ECOG study or a similar European (GETUG-AFU 15) trial."

The current ASCO guidelines state: "Recommendation 1.2. For patients with low-volume metastatic disease (LVD) as defined per CHAARTED who are candidates for chemotherapy, docetaxel plus ADT should not be offered (Type: evidence-based, benefits outweigh harms; Evidence quality: high; Strength of recommendation: strong for patients with LVD)."

On the other hand, the current AUA/ASTRO/SUO guidelines state: "15. In patients with mHSPC, clinicians should offer continued ADT in combination with either androgen pathway directed therapy (abiraterone acetate plus prednisone, apalutamide, enzalutamide) or chemotherapy (docetaxel). (Strong Recommendation; Evidence Level: Grade A)

Canadian Urological Assn (CUA) guidelines state: "Docetaxel plus ADT may also be an option in patients with mCNPC/mCSPC with good performance status with low-volume disease (Level 2, Weak recommendation)."

NICE (UK) guidelines state: "Offer docetaxel chemotherapy to people with newly-diagnosed metastatic prostate cancer who do not have significant comorbidities."

European Urological Assn (EAU) guidelines state: "Based on these data, upfront docetaxel combined with ADT should be considered as a standard in men presenting with metastases at first presentation provided they are fit enough to receive the drug [1070]"

I personally believe that the STAMPEDE researchers make a stronger case pending better data from PEACE1.

Thank you again for taking time to reply to me.

AlanMeyer profile image
AlanMeyer in reply toSkipper238

Hello Skipper,

The first thing I want to say about your response is that I am deeply impressed by the effort you are making to understand the medical/scientific and personal/family issues you are confronting. The science is complicated, difficult, and inexact. The personal issues are full of unknowns. I think you're doing better than most of us in trying to figure it all out.

I used to imagine that I understood all of the science as well as any of us patients did until Tall Allen joined the group and I realized how much more he read, studied, and understood the science than I did. I try to be more circumspect now in my pronouncements about treatment. However, bearing in mind that everything I say is based on inadequate study and should not be taken as authoritative (something that I('m sure you won't do) I will add a few ideas about your analysis above.

The first is that the studies of ADT + abiraterone or docetaxel found that, for the category of men that were helped by them, the combination of ADT + one of the other drugs taken at the same time produced significantly longer life than ADT followed by one of the other drugs after ADT failed. I presume that happened because the tumor population was more successfully suppressed than happened with ADT alone. The number of cells that developed resistance to both treatments at once would have been much smaller than those cells developing resistance to either one by itself.

A second point I want to make here is that both abiraterone and docetaxel are drugs that are administered over time. If you take a dose of one of them and face intolerable adverse effects, I think it should be possible to simply discontinue the drugs, switch to another concomitant treatment, or fall back on ADT alone. Most of the adverse effects should disappear in not too many days after discontinuing treatment. Consult your oncologists about this - they'll have experience with men who have done that. I don't think it should be necessary to rule out advanced treatment before you've tried it.

There are many men on this forum who have managed abiraterone and/or docetaxel and concluded that the benefit was much greater than the harm. There are, or course, others who had the opposite experience.

In some cases I believe that the management of treatment has something to do with the experience of side effects. For example some men may be given 1/2 or 1/3 the normal dose of docetaxel but twice or three times as often as the normal dose so that their total dosage is that same. The one paper I read about that said that side effects were reduced without reducing the treatment effect. The one patient who told me about his experience with altered dosage claimed he had no significant side effects from docetaxel but his treatment response was excellent. Some men are offered cold baths for hands, feet, head, and mouth to reduce side effects there, Other men are not offered that. Some men are offered Neulasta to help avoid infections. Others are not.

Best of luck.

Alan

treedown profile image
treedown

I had both enlarged and mildly prominent lymph nodes noted on my original CT scan. I started Lupron right away and talked to my RO 2 months later. He decided to get a biopsy of a distant mildly prominent lymph node prior to radiation. They could not find a lymph node at all with ultrasound. They thought they did, doped me up, then tried to find it again for 20 minutes. 3 people tried and they weren't able to find any lymph nodes and gave up. Seems like this procedure should have been done before ADT but it once diagnosed they want you on the ADT train right away. They proceeded to radiate me up to my aortic bifurcation which is as high as they normally go. My PSA was 156 with relatively low Gleason, clean bone scan and only assumed (rightly so IMO) LN involvement so from day one all docs were convinced I have more cancer than could be seen. So if your treatment is effective after a couple months of ADT I suspect they won't find much in your lymph nodes. Not sure if that is a good thing or a bad thing anymore but time may tell.

Good luck to you and mat all your treatments have longterm success.

Skipper238 profile image
Skipper238 in reply totreedown

Thank you, Treedown. One thing I am trying to sort out is exactly this. It seems like taking a biopsy now is a good idea. "Tall" pointed out a couple of reasons in his post. I don't understand the issues well enough to know, right now. My question has to do with the biopsy report from prostate biopsy. Does it have enough cell information and "histological" data that if my lymph nodes do shrink after 60 days of ADT, no biopsy is really needed? Or, is there more to be learned, even at that point, by taking a biopsy of the lymph nodes. I will figure this out and ask my Oncologist more about it at my appointment on Dec. 30. I don't get my first Eligard shot until this Friday, Dec. 10, so there should still be enough lymph node around at that time, if a decision is made to do a biopsy.

Thank you.

treedown profile image
treedown in reply toSkipper238

My RO was trying to biopsy a LN to determine how high/much to radiate. He wanted to get beyond the, for lack of a better word, "known" cancer. I researched LN size as mine were enlarged but still not giant and that research noted that mine were not abnormally large. After the biopsy attempt I had a pelvic MRI and that confirmed my LN had shrunk. The whole process takes time and wrapping my head around everything is an ongoing process. I have learned to let things come as they may and deal with them at that time. All the energy I was using to predict or anticipate has proven to be misdirected in many ways. Now I just try to absorb and learn. This forum is great and I would feel far more lost without it.

Skipper238 profile image
Skipper238 in reply totreedown

Thanks very much. I'm on the phone right now with MD Anderson, scheduling my appointment for a second opinion on treatment. We see what the good doctors at MD Anderson have to say.

2dee profile image
2dee

Actually you have gotten things going pretty well.Get multiple opinions from PCa specialists, continue your self education so you can ask and discuss all your options.

Don't relent from your goal of living longer than anyone thought possible.

Exercise diligently, enjoy your family and friends.

Follow the SOC Standard Of Care. It is based on the best treatments that science can offer.

Seek out a local support group and monitor HU daily. Learn from the posts and the responses.

2Dee

Skipper238 profile image
Skipper238 in reply to2dee

Thank you, 2dee. I appreciate that. Please let me know what "Hu" stands for. Thank you.

Shermanhill profile image
Shermanhill in reply toSkipper238

HU = this site (Health Unlocked).

larry_dammit profile image
larry_dammit

Don’t wait, get into Md Anderson and get aggressive treatment. The sooner you do the longer you will live. Never give in warrior 🙏🙏🙏

DesertDaisy profile image
DesertDaisy

My husband was diagnosed with prostate cancer in November 2020. It was a very confusing time for us and we didn't know where to turn. We ended up at Mayo Clinic in Phoenix and have been very pleased with his care there. Since you are going to Jacksonville, it may be good to also schedule a consultation at Mayo.

Skipper238 profile image
Skipper238 in reply toDesertDaisy

Thank you.

Skipper238 profile image
Skipper238

Thank you, but I am quite committed to the medical route. Best to you.

Scout4answers profile image
Scout4answers

Hi iyoder I have taken the SOC route as well but would also like to hear what you are doing as I am contemplating a more natural approach once the ADT phase ends.

Scout

CurrentSEO profile image
CurrentSEO in reply toScout4answers

iyoder promoting some mambo jumbo supplement PC HOPE, that is latest reincarnation of PC-SPES (was banned by FDA because contained hormones and other non-declared prescription meds) with unknown content from ugly looking sales pitch website. He most likely behind it. That is my opinion of course.

CAMPSOUPS profile image
CAMPSOUPS in reply toCurrentSEO

I totally agree with your opinion. I will go a bit further. The poster is a hack.Look at his posts and replies on his bio page.

There is one agenda and one agenda only which is to promote the Nutrition2000 business which as you noted was flagged by the FDA.

Its insidious to find a site like this and prey on desperate people.

I dont know why it pisses me off so much but it does.

Scout4answers profile image
Scout4answers in reply toCurrentSEO

Buyer beware...Here is what NIH says:

PC-SPES (PDQ®)–Patient Version

Go to Health Professional Version

ON THIS PAGE

Overview

Questions and Answers About PC-SPES

About This PDQ Summary

General CAM Information

Evaluation of CAM Therapies

Questions to Ask Your Health Care Provider About CAM

To Learn More About CAM

Overview

NOTE: The information in this summary is no longer being updated and is provided for reference purposes only.

PC-SPES is a mixture of 8 herbs that was sold as a dietary supplement to keep the prostate healthy (see Question 1).

Some batches of PC-SPES were found to contain prescription medicines. It was taken off the market and is no longer being made (see Question 1).

Herbs in PC-SPES have been used in traditional Chinese medicine for many health problems, including prostate problems, for hundreds of years (see Question 2).

The herbs used in PC-SPES have been reported to help keep cancer cells from growing or help prevent cell damage that can lead to cancer (see Question 3).

Laboratory and animal studies suggested that PC-SPES might slow the growth of prostate cancer cells, but it is not known if these results were caused by the herbs in PC-SPES, prescription medicines that were found in the mixture, or both (see Question 5).

Clinical trials suggested that PC-SPES lowers PSA (prostate specific antigen) and testosterone levels in humans and has some anticancer effects. It is not known if these results were caused by the herbs in PC-SPES, prescription medicines that were found in the mixture, or both (see Question 6).

The U.S. Food and Drug Administration has not approved PC-SPES for use in cancer treatment (see Question 8).

Questions and Answers About PC-SPES

What is PC-SPES?

PC-SPES is a mixture of herbs that was sold as a complementary and alternative medicine (CAM) treatment for people with prostate cancer. The mixture contains these 8 herbs:

Baikal skullcap (Scutellaria baicalensis)

Chrysanthemum flowers (Dendranthema morifolium)

Reishi mushroom (Ganoderma lucidum)

Isatis (Isatis indigotica)

Licorice (Glycyrrhiza glabra or Glycyrrhiza uralensis)

Ginseng (Panax ginseng or Panax pseudoginseng var. notoginseng)

Rabdosia rubescens (Isodon rubescens)

Saw palmetto (Serenoa repens)

PC-SPES was taken off the market because some batches were found to contain prescription medicines in addition to the herbs. Clinical trials of PC-SPES that were underway were stopped. There are products being sold now as substitutes for PC-SPES, but they are not the same mixture. Since the only company licensed to make PC-SPES is no longer in business, PC-SPES is not legally available in the United States.

What is the history of the discovery and use of PC-SPES as a complementary and alternative treatment for cancer?

Most of the herbs in PC-SPES have been used in traditional Chinese medicine (TCM) for many health problems, including prostate problems, for hundreds of years. A chemist in New York and a doctor/herbalist in China worked together to create the mixture. In 1997, a company was formed to make PC-SPES and sell it in the United States without a prescription. Interest in PC-SPES grew, and researchers began looking at it. Tests found that some batches of PC-SPES contained one or more of the following drugs, which are not found in nature:

DES, a type of estrogen made in a lab.

Warfarin (Coumadin), a blood-thinner.

Indomethacin, a drug used to decrease inflammation.

Because these drugs are to be used only by prescription and could be harmful to some people, PC-SPES was taken off the market in 2002.

What is the theory behind the claim that PC-SPES is useful in treating cancer?

In lab tests, each herb used in PC-SPES has been reported to help keep cancer cells from growing or to help prevent cell damage that can lead to cancer and other diseases.

PC-SPES was reported to slow the growth of prostate cancer but did not cure it. It is not known how PC-SPES works in the body. Some of the herbs in the mixture contain phytoestrogens, which are estrogen-like substances found in plants. Estrogen can cause the testicles to stop making testosterone, which makes some prostate cancers grow. Patients' responses to PC-SPES were similar to responses to estrogen therapy using DES. The DES found in some batches of PC-SPES, however, may not have been enough to cause all of the estrogen-like effects that were seen in users of the mixture. There is some evidence that the mixture works in a different way than DES does, and that PC-SPES alone (without DES in it) may fight prostate cancer.

PC-SPES has also shown anticancer effects on prostate cancers that do not depend on testosterone and on other types of cancer. This suggests that PC-SPES may have anticancer qualities other than its estrogen-like effects.

How is PC-SPES administered?

PC-SPES is taken by mouth in capsules.

Have any preclinical (laboratory or animal) studies been conducted using PC-SPES?

Studies of PC-SPES in test tubes and using rats showed that it might keep cancer cells from growing. These studies were done, however, before it became known that some batches of the product contained unlisted prescription medicines. Also, the product was not standardized (different batches of PC-SPES were found to contain different strengths of the herbal ingredients). For these reasons, the results of the lab tests and animal studies are not considered to be good evidence.

Have any clinical trials (research studies with people) of PC-SPES been conducted?

Clinical trials of PC-SPES had begun before the product was taken off the market. In these trials, PC-SPES was reported to improve quality of life, reduce pain, and lower PSA (prostate specific antigen) levels in patients with prostate cancer. Rising PSA levels can be a sign that prostate cancer is growing.

After it was learned that some batches of PC-SPES contained prescription medicines, ongoing studies were stopped and previous study results came into question. The responses reported in the studies may have been caused by the prescription medicines that were in the PC-SPES, as well as by the herbal ingredients. Also, since different batches of PC-SPES contained different ingredients, the studies cannot easily be compared.

Have any side effects or risks been reported from PC-SPES?

Common side effects were the same as those reported with estrogen therapy:

Breast swelling and tenderness.

Loss of sex drive.

Impotence (inability to have an erection).

There were other, less common, side effects:

Blood clots in the legs.

Diarrhea.

PC-SPES may also change the way drugs, including anticancer drugs, work in the body. It may cause drugs to be more or less effective, or cause effects on the body that are not expected.

Is PC-SPES approved by the U.S. Food and Drug Administration (FDA) for use as a cancer treatment in the United States?

The U.S. Food and Drug Administration has not approved PC-SPES for use in cancer treatment. It is not legally sold in the United States.

About This PDQ Summary

About PDQ

Physician Data Query (PDQ) is the National Cancer Institute's (NCI's) comprehensive cancer information database. The PDQ database contains summaries of the latest published information on cancer prevention, detection, genetics, treatment, supportive care, and complementary and alternative medicine. Most summaries come in two versions. The health professional versions have detailed information written in technical language. The patient versions are written in easy-to-understand, nontechnical language. Both versions have cancer information that is accurate and up to date and most versions are also available in Spanish.

PDQ is a service of the NCI. The NCI is part of the National Institutes of Health (NIH). NIH is the federal government’s center of biomedical research. The PDQ summaries are based on an independent review of the medical literature. They are not policy statements of the NCI or the NIH.

Purpose of This Summary

This PDQ cancer information summary has current information about the use of PC-SPES in the treatment of people with cancer. It is meant to inform and help patients, families, and caregivers. It does not give formal guidelines or recommendations for making decisions about health care.

Reviewers and Updates

Editorial Boards write the PDQ cancer information summaries and keep them up to date. These Boards are made up of experts in cancer treatment and other specialties related to cancer. The summaries are reviewed regularly and changes are made when there is new information. The date on each summary ("Updated") is the date of the most recent change.

The information in this patient summary was taken from the health professional version, which is reviewed regularly and updated as needed, by the PDQ Integrative, Alternative, and Complementary Therapies Editorial Board.

Clinical Trial Information

A clinical trial is a study to answer a scientific question, such as whether one treatment is better than another. Trials are based on past studies and what has been learned in the laboratory. Each trial answers certain scientific questions in order to find new and better ways to help cancer patients. During treatment clinical trials, information is collected about the effects of a new treatment and how well it works. If a clinical trial shows that a new treatment is better than one currently being used, the new treatment may become "standard." Patients may want to think about taking part in a clinical trial. Some clinical trials are open only to patients who have not started treatment.

Clinical trials can be found online at NCI's website. For more information, call the Cancer Information Service (CIS), NCI's contact center, at 1-800-4-CANCER (1-800-422-6237).

Permission to Use This Summary

PDQ is a registered trademark. The content of PDQ documents can be used freely as text. It cannot be identified as an NCI PDQ cancer information summary unless the whole summary is shown and it is updated regularly. However, a user would be allowed to write a sentence such as “NCI’s PDQ cancer information summary about breast cancer prevention states the risks in the following way: [include excerpt from the summary].”

The best way to cite this PDQ summary is:

PDQ® Integrative, Alternative, and Complementary Therapies Editorial Board. PDQ PC-SPES. Bethesda, MD: National Cancer Institute. Updated <MM/DD/YYYY>. Available at: cancer.gov/about-cancer/tre.... Accessed <MM/DD/YYYY>. [PMID: 26389430]

Images in this summary are used with permission of the author(s), artist, and/or publisher for use in the PDQ summaries only. If you want to use an image from a PDQ summary and you are not using the whole summary, you must get permission from the owner. It cannot be given by the National Cancer Institute. Information about using the images in this summary, along with many other images related to cancer can be found in Visuals Online. Visuals Online is a collection of more than 3,000 scientific images.

Disclaimer

The information in these summaries should not be used to make decisions about insurance reimbursement. More information on insurance coverage is available on Cancer.gov on the Managing Cancer Care page.

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More information about contacting us or receiving help with the Cancer.gov website can be found on our Contact Us for Help page. Questions can also be submitted to Cancer.gov through the website’s E-mail Us.

General CAM Information

Complementary and alternative medicine (CAM)—also called integrative medicine—includes a broad range of healing philosophies, approaches, and therapies. A therapy is generally called complementary when it is used in addition to conventional treatments; it is often called alternative when it is used instead of conventional treatment. (Conventional treatments are those that are widely accepted and practiced by the mainstream medical community.) Depending on how they are used, some therapies can be considered either complementary or alternative. Complementary and alternative therapies are used in an effort to prevent illness, reduce stress, prevent or reduce side effects and symptoms, or control or cure disease.

Unlike conventional treatments for cancer, complementary and alternative therapies are often not covered by insurance companies. Patients should check with their insurance provider to find out about coverage for complementary and alternative therapies.

Cancer patients considering complementary and alternative therapies should discuss this decision with their doctor, nurse, or pharmacist as they would any type of treatment. Some complementary and alternative therapies may affect their standard treatment or may be harmful when used with conventional treatment.

Evaluation of CAM Therapies

It is important that the same scientific methods used to test conventional therapies are used to test CAM therapies. The National Cancer Institute and the National Center for Complementary and Integrative Health (NCCIH) are sponsoring a number of clinical trials (research studies) at medical centers to test CAM therapies for use in cancer.

Conventional approaches to cancer treatment have generally been studied for safety and effectiveness through a scientific process that includes clinical trials with large numbers of patients. Less is known about the safety and effectiveness of complementary and alternative methods. Few CAM therapies have been tested using demanding scientific methods. A small number of CAM therapies that were thought to be purely alternative approaches are now being used in cancer treatment—not as cures, but as complementary therapies that may help patients feel better and recover faster. One example is acupuncture. According to a panel of experts at a National Institutes of Health (NIH) meeting in November 1997, acupuncture has been found to help control nausea and vomiting caused by chemotherapy and pain related to surgery. However, some approaches, such as the use of laetrile, have been studied and found not to work and to possibly cause harm.

The NCI Best Case Series Program which was started in 1991, is one way CAM approaches that are being used in practice are being studied. The program is overseen by the NCI’s Office of Cancer Complementary and Alternative Medicine (OCCAM). Health care professionals who offer alternative cancer therapies submit their patients’ medical records and related materials to OCCAM. OCCAM carefully reviews these materials to see if any seem worth further research.

Questions to Ask Your Health Care Provider About CAM

When considering complementary and alternative therapies, patients should ask their health care provider the following questions:

What side effects can be expected?

What are the risks related to this therapy?

What benefits can be expected from this therapy?

Do the known benefits outweigh the risks?

Will the therapy affect conventional treatment?

Is this therapy part of a clinical trial?

If so, who is the sponsor of the trial?

Will the therapy be covered by health insurance?

To Learn More About CAM

National Center for Complementary and Integrative Health (NCCIH)

The National Center for Complementary and Integrative Health (NCCIH) at the National Institutes of Health (NIH) facilitates research and evaluation of complementary and alternative practices, and provides information about a variety of approaches to health professionals and the public.

NCCIH Clearinghouse

Post Office Box 7923 Gaithersburg, MD 20898–7923

Telephone: 1-888-644-6226 (toll free)

TTY (for deaf and hard of hearing callers): 1-866-464-3615

E-mail: info@nccih.nih.gov

Website: nccih.nih.gov

CAM on PubMed

NCCIH and the NIH National Library of Medicine (NLM) jointly developed CAM on PubMed, a free and easy-to-use search tool for finding CAM-related journal citations. As a subset of the NLM's PubMed bibliographic database, CAM on PubMed features more than 230,000 references and abstracts for CAM-related articles from scientific journals. This database also provides links to the websites of over 1,800 journals, allowing users to view full-text articles. (A subscription or other fee may be required to access full-text articles.)

Office of Cancer Complementary and Alternative Medicine

The NCI Office of Cancer Complementary and Alternative Medicine (OCCAM) coordinates the activities of the NCI in the area of complementary and alternative medicine (CAM). OCCAM supports CAM cancer research and provides information about cancer-related CAM to health providers and the general public via the NCI website.

National Cancer Institute (NCI) Cancer Information Service

U.S. residents may call the Cancer Information Service (CIS), NCI's contact center, toll free at 1-800-4-CANCER (1-800-422-6237) Monday through Friday from 9:00 am to 9:00 pm. A trained Cancer Information Specialist is available to answer your questions.

Food and Drug Administration

The Food and Drug Administration (FDA) regulates drugs and medical devices to ensure that they are safe and effective.

Food and Drug Administration

10903 New Hampshire Avenue

Silver Spring, MD 20993

Telephone: 1-888-463-6332 (toll free)

Website: fda.gov

Federal Trade Commission

The Federal Trade Commission (FTC) enforces consumer protection laws. Publications available from the FTC include:

Who Cares: Sources of Information About Health Care Products and Services

Fraudulent Health Claims: Don’t Be Fooled

Consumer Response Center

Federal Trade Commission

600 Pennsylvania Avenue, NW

Washington, DC 20580

Telephone: 1-877-FTC-HELP (1-877-382-4357) (toll free)

TTY (for deaf and hard of hearing callers): 202-326-2502

Website: ftc.gov

Updated: January 7, 2015

slpdvmmd profile image
slpdvmmd

Your story sounds somewhat similar to my own. I was lucky enough to be evaluated early by a multidisciplinary team with a very progressive medical oncologist who advised that I start on ADT, docetaxel (6 cycles), abiraterone/pred and use radiation for local control right out of box. He was aware of the on-going trial which later resulted in the paper cited by TallAllen and was a strong advocate for me getting this approved by my insurer. The evolution of prostate cancer care seems to be away from just adding something on as you PSA bumps but instead to be aggressive out of the box. The one error I think in my care was that I did not follow up immediately on completion of my chemo and radiation with a PSMA PET/CT as I had a high grade tumor and the odds of it being positive and amendable to Lutetium "mopup" were high.

MateoBeach profile image
MateoBeach

A big question that has not been adequately answered is whether or not those abnormal lymph nodes are actually prostate cancer. F18 PET scan does not answer that. You could wait to see if the ADT shrinks them. Personally, I would insist on a PSMA specific PET scan such as Pylarify. If that shows them to be PSMA avid then it confirms it. And also prepares you for taking advantage of Lu-PSMA treatment which is expected to be approved soon. Also, if that is positive, then you are “de-novo metastatic PC and have “high burden” if more than 4 nodes are positive. That would indicate you may benefit from the triple early regimen of the PEACE-1 trial.I would have this sorted out at MD Anderson place of your choice. I would not be deterred about flying to Houston, in person visit, etc. Just be fully vaccinated and very consistent with mask wearing, hand sanitizer, etc. Yes your life depends on choosing wisely with the best medical team. Perhaps they can pre-schedule you for the PSMA PET scan at MDA the same day as your consult. Keep good relations with your current local doctors. You may need services through them once the plan is in place.

Skipper238 profile image
Skipper238 in reply toMateoBeach

Thank you, Mateo. I have scheduled a consultation/second opinion for my treatment with the good doctors at MD Anderson in Jacksonville, FL. I will add this to my list to discuss with them. I appreciate your post and suggestion on the PSMA-specific PET. I'm curious to know how much is spread within my body anyway. Thank you.

j-o-h-n profile image
j-o-h-n

Greetings Skip,

T_A knows his shit...........So do many other guys on here....(I don't)....

Good Luck, Good Health and Good Humor.

j-o-h-n Wednesday 12/08/2021 7:30 PM EST

Skipper238 profile image
Skipper238 in reply toj-o-h-n

Thanks, John. I can see that The Tall one is the real deal. Thx. 😀👍

LowT profile image
LowT

Comment: All cancers occur in a unique context, I.e. the patient. You have not mentioned anything about your overall health status. I assume you have a good and experienced internal medicine physician. Medical care is very fragmented today and it is critical to address the whole patient. Also it’s great to be a model man’s man for your children but that also includes being human. No need to go through all this alone. Be open to vulnerability and human emotions. It’s all part of life. We all need each other. We all deserve that. You’ve done a remarkable job at educating yourself. Very impressive. You are receiving priceless knowledge from those on this group. Stay connected.

Skipper238 profile image
Skipper238 in reply toLowT

Hi LowT,

Thanks for your thoughts. I am trying to assemble a good team of doctors to help me with all of this. That is currently a work in progress.

In terms of being a "model man's man" for my children's sake, as you put it, that is really not my goal. I don't think in those terms. Rather, I think in terms of what I think is best for my children. If you look at my post about using a packet of frozen corn to help numb the injection site for my first Eligard treatment, you'll see evidence of that I'm not focused on being a "man's man" :). (Also, I just used a smiley face in a sentence, so hey, there you go. A man's man does not EVER use a smiley face in a sentence!

With my children, I am making every effort to not overly focus on my advance prostate cancer and to providing clear, sensitively communicated and age-appropriate info. What I am trying to prevent, as I am sure many before me have done, is t my children starting to worry NOW about the severity, permanence and end of life considerations for my condition. Said simply, I don't want them to think I'm about to die.

I want to let my new reality of having advanced PC roll for a while -- let it unfold -- as I begin the best treatment possible. Over time, my children will see how I am doing, which hopefully will be encouraging for them. In the future, if I take a turn for the worse, I may find it important to education them more and be more specific about "things".

But, right now, I am focused on getting my treatment plan in order and then getting back to living. There will come a time for dying, but that time is not now. So, again, simply put, right now I say it to my kids a bit like this: "Kids, It turns out I do have prostate cancer, but it is treatable. I'll need to take medicine for the rest of my life, probably, but as we know, we're all lucky to be living in a time where medical science is improving every day. We can talk as much as you'd like, but I'm good."

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