Effect of High SUV, etc on staging survival percentages - 1289454

Me53,

I am not a doctor but since being diagnosed and treated I've read a lot about lung cancer.

Any % figure you are quoting for stage IIIb is lumping in a vast variety of different situations including, in particular, people who are not operated on, degrees of lymph node invasion and other aspects of the disease -- all considered 3B but actually different, like your adenosquamous.

I also know that SUV max goes up with stage so having an SUV max of 11 may be average or low for stage IIIb, rather than high. (I don't know). When people write that something is unfavorable, well that is already taken into account in the IIIb diagnosis, that those tend to be more aggressive tumors than e.g. stage 1.

ADS is not something I know much about. Did you have chemo?

That SUV may be independently correlated does not address whether your SUV is high or low compared to average for the stage. Also many if not most stage 3B are not resected and that has a big effect on survival.

Have you had chemo?

Are you seen by an expert in adenosquamous. Have you been tested for genetic markers?

From what I can tell adenosquamous is really its own beast. Here is a paper on prognosis factors. Post operative chemo is a favourable factor, so is predominant squamous vs. predominant adeno. It's a small study, but it is recent. There are others
Clinicopathological characteristics and prognosis of patients with adenosquamous lung carcinoma

Volume: 35 Issue: 3 Pages: 350-355
DOI: 10.1007/s11596-015-1436-z
Published: JUN 2015
Abstract
This study was aimed to characterize clinicopathological features and prognosis of patients with adenosquamous lung carcinoma (ASC). Among the 2531 patients with lung cancer who underwent surgery between January 2000 and June 2012 in our hospital, 59 were histologically diagnosed as having ASC. The clinicopathological features and follow-up data of ASC patients were collected and analyzed statistically. Superior lobectomy was accomplished in 40 patients, middle and inferior lobectomy in 3, lobectomy plus partial resection of contralateral lung in 5, partial lung resection in 4, and pneumonectomy in 7. Moreover, 22 cases were found to be adenocarcinoma-predominant, and 18 to be squamous cell carcinoma-predominant. The median survival time was 13.6 months, and the 1-, 3-, and 5-year survival rates were 59.9%, 36.4% and 31.2%, respectively. Of the 52 cases with tissue specimens available, 11 had an EGFR mutation (21.2%) and 2 had a KRAS mutation (3.8%). Multivariate analysis showed that histology subtype, pleural invasion, TNM stage, and postoperative treatment were all independent prognostic factors. The data from the current study demonstrated that SCC-predominant histology represents a better prognosis of ASC. Histology subtype,
pleural invasion, TNM stage, and postoperative treatment are independent prognostic factors for ASC and adjuvant therapy may help control the disease.

If you have not already seen it, perhaps this study will be helpful: http://www.atsjournals.org/doi/full/10.1513/pats.200806-059LC

In this retrospective analysis of various trials, the difficulty of isolating one particular factor is noted, including the varying thresholds used to define "high SUV". There is also discussion of how prognosis can vary based on tumor type and differentiation, as well as the magnitude of decrease in SUV following treatment with chemotherapy or chemoradiation.

JimC
Forum moderator

Let me preface this with: If someone has input pertaining please do leave a comment for we still have an unanswered question.

me53,

I'm sorry but I don't think we (forum moderators or oncology facalty) will be able to answer your question. We've tried. We just aren't equipped to answer questions about prognosis past what you've already dug up. Dr. Weiss gave us time and input to no use to you nor did Jim or I or other members provide the prognostic info you need. We are always willing to help with input but there are obvious limits to our forum. I'm sorry our attempts feel like we don't respect your legitimate need to know. As Dr. Weiss stated before, "I’m afraid that I don’t have a lot to add that directly answers the subject under discussion, prognostication. As an oncologist, I have spent little time on vetting the literature and doing research on prognosis (which means factors that predict outcome regardless of choices made). To the contrary, I’ve spent more time on prediction (which means markers that help guide the right thing to do). I understand from a human standpoint why you are interested in everything that you can learn re prognosis, but can’t help much." http://cancergrace.org/topic/importance-of-prognosis-markers/#post-1289…

If you find what your looking for please do share with us. If you find that you need other info give us a try again.

All best,
Janine

Is this helpful? "Intracytoplasmic mucin is associated with specific clinical characteristics and is an independent factor for worse survival in lung adenocarcinoma formerly known as BAC. http://www.lungcancerjournal.info/article/S0169-5002(14)00004-X/abstrac…
It's only a piece of your personal puzzle though.

There may be someone associated with this trial that may be willing to help you. https://clinicaltrials.gov/ct2/show/NCT00759382?term=suv%2C+Prognostic+…

I think the moderators have gone out of their way to provide relevant information.

It is not at all clear that SUV max is prognostic for stage III lung cancer. Here is a recent, serious study that says it is not. Other finding from PET are, however.

Pretreatment PET and Overall Survival
At the time of database locking, median survival time after study registration was 19.9 months, and 159 patients (74.3%) had died. Univariate Cox proportional hazards testing revealed that pretreatment MTV (HR = 1.04 per 10cm3 increase, 95% CI = 1.03 to 1.06, P < .001) and pretreatment TGA (HR = 1.33 per natural log increase, 95% CI = 1.15 to 1.54, P < .001) were statistically significant predictors of mortality, while SUVmax was not prognostic (HR = 1.01, 95% CI = 0.99 to 1.03, P = .38)."

Pretreatment FDG-PET Metrics in Stage III Non–Small Cell Lung Cancer: ACRIN 6668/RTOG 0235
http://jnci.oxfordjournals.org/content/107/4/djv004.full

me53,

I am sorry that you feel that we have not made good faith attempts to respond to your question; I don't think we will be able to provide you with the answer you seek. In this post I will try to explain in some detail why we have been responding as we have. Therefore, this post will not provide you with an answer, so please feel free to stop reading at this point.

As you describe, the five-year survival rate for stage IIIb lung cancer is around 9 percent, but it includes three broad categories of patients. First, there are those whose cancer never recurs after initial surgery and/or chemoradiation. Second, there are patients whose cancer recurs locally but through subsequent treatment is eliminated or kept in check to at least the five-year mark. Third, some patients' cancers will recur and spread distantly, making them stage IV, but treatment may also control these cancers to the five-year point. It's not simply that 91 percent recur or metastasize and don't make it, while 9 percent will neither recur nor metastasize and will survive.

Each of these patients will contribute to the 9 percent statistic, and the recent advances of which you speak will be most helpful to those in the second two groups, as chemotherapy agents and radiation techniques have improved. That is why I cited the study that I did, despite its age. One of the conclusions is that higher SUV may not be as relevant as response to treatment and degree of reduction in SUV post-treatment. The only element that may have changed is that better therapies may have increased the number of patients whose cancer is controlled and whose SUV has significantly decreased. The response to subsequent treatment remains a more important factor, according to that meta-analysis.

[continued in following post]

[continued from previous post]

In your situation, a relatively high SUV is a negative prognostic factor. It probably increases your chance of recurrence. But so far, your cancer has not recurred, and that is terrific; the longer you go without recurrence, the better your chance to reach five-year survival. If you do recur, your response to treatment will be critical. If you are eight months out from surgery, your chances likely are already better than 9 percent, since one would expect a particularly aggressive cancer to recur sooner rather than later.

You have stated that you have read recent studies linking high SUV with decreased survival, although you no longer have the links, but that Dr. West or other medical professionals would/should be familiar with them. I will respectfully disagree with you on this point. Oncologists review many studies, but they focus on the conclusions which may have an effect on clinical practice and/or further research. The effect of a particular marker/factor tends to be looked at in terms of median time to progression or median survival rather than a percentage chance of reaching five years. For example, if a patient is two years out from surgery, no matter what the initial SUV that patient's chance of five-year survival is most likely much higher than 9 percent, as the risk of recurrence drops significantly as time goes on. As Dr. Weiss stated, such a study might only be critical to oncology practice in the sense that it may dictate treatment choices. If you had links, it would be easier for us to provide some interpretation, but since the doctors here contribute their time without charge, it is not practical for them to spend large amounts of their time to find those particular studies.

[continued in the following post]

[continued from previous post]

That is why the discussion turned to adjuvant therapy; the higher SUV may lead to a certain choice of treatment. For example, a high SUV in a stage II resected tumor will make adjuvant therapy more advisable, although the same risk/benefit considerations you faced would also apply. Since you had already very reasonably declined adjuvant therapy, your non-recurrence is now a much more significant factor, and if you do recur, your response to treatment will be as well.

Several years ago our friend Neil, one of the original GRACE moderators, posted this non-scientific take on survival statistics: http://cancergrace.org/forums/index.php?topic=826.msg4326#msg4326

Please do not feel any need to respond if you feel that this information duplicates what already has been provided.

JimC

The 5 year survival rate of stage 3B lung cancer is not 9% as has been erroneously reported in this thread. I hope whoever might stumble across this wouldn't get unduly discouraged by this incorrect information.

According to the "The IASLC Lung Cancer Staging Project: Proposals for Revision of the TNM Stage Groupings in theForthcoming (Eighth) Edition of the TNMClassification for Lung Cancer"

report in 2016, the 5 year survival rate of stage 3B lung cancer is

19% (according to 7th edition criteria)
26% (according to 8th edition criteria)

The eight edition made some changes including introducing the new category stage 3C, which has lower survival. This is why survival for 3B went up in 8th ed. compared to 7th.

I know about these changes because my category also changed for different reasons.

https://www.ncbi.nlm.nih.gov/pubmed/26762738

ME53, if you want to challenge this please provide a publication for reference.

I have already posted a paper that shows that SUV max is not prognostic in stage 3 lung cancer. Indeed there are other recent papers showing the same. However other features of pre-treatment PET are found to be prognostic for stage III but not SUV max. You have not posted any papers to justify your claims. Why don't you read the paper I posted?

About the large database giving the survival stats for the 7th edition and 8th edition Stage IIIB (7th would have been in place in 2015) this is it:

"The new IASLC database has information on 94,708 new patients diagnosed of lung cancer between 1999 and 2010. They originated from 35 sources in 16 countries, and 4,667 were submitted via the online electronic data capture system. Europe contributed 46,560 patients, Asia: 41,705, North America: 4,660, Australia: 1,593, and South America: 190. After exclusions, 77,156 (70,967 with nonsmall cell lung cancer and 6,189 with small cell lung cancer) remained for analysis. This database will be analyzed according to established objectives for the T, the N, and the M components to inform the eighth edition of the TNM classification of lung cancer due to be published in 2016. "

https://www.ncbi.nlm.nih.gov/pubmed/25436796

Again you have not posted any paper to justify your use of 9% survival.

Maybe this is good news for you?

I cannot give you exact numbers, nor do I believe anyone can, because there are not large studies of people that get as granular as your question. Current staging analyses that provide prognostic assessments do not include either PET SUV or intracellular mucin because these are not reliable indicators in large studies, even if they are factors that tend to be associated with a worse prognosis.

I would consider it very likely that with T4 disease, very PET-avid disease in more than one node, the probability of recurrence is quite high -- not 100%, but likely higher than 90-95%. I don't think it's possible to put a finer point on it -- there just aren't data on populations of patients with T4, high SUV, adenosquamous NSCLC to guide expectations.

Good luck.
-Dr. West

The trials basically show that, stage for stage, patients with a poorly differentiated cancer and/or high SUV tend to do worse. I don't know that you can say that a high SUV accounts for a death rate, but there's a definite correlation -- it just hasn't been precisely quantified. It is fair to say that a low SUV on PET tends to go with a more indolent pattern of progression and longer survival, while a higher SUV is associated with a more rapid rate of progression, higher risk of recurrence in earlier stage, etc. -- it's just that there are definitely people with a high SUV cancer who never have their cancer recur after surgery or chemo/radiation, etc.

-Dr. West