mBAC / AIS and immunotherapy nivolumab - 1290307

Thank you Jim for your kind wishes and thanks for the podcast link.
NSCLC is a rather broad definition of LC. There may be quite some meaningful variety among the subgroups that will affect the extent of the response.
Apparently, KEYTRUDA trials were based on narrower parameters for the subgroups than OPDIVO and as such were more successful because they found a better fitting subgroup. (http://blogs.sciencemag.org/pipeline/archives/2016/10/10/keytruda-vs-op…).
We have neither tissue left not can we do another biopsy since too risky after my wife's lobectomy. So KEYTRUDA at this point was not in the picture.
There is also an study on neutrophils (https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5296654/). I am not schooled in this area but to me it suggests that targeting just NSCLC is painting with too broad a brush. Targeting smaller subgroups may find better fits but then the cost-benefit of such research comes into play.
Over the past six years we have been fortunate that the Carbo-Alimta kept it stable for more than two years, the docetaxel for less than a year. It did work but side effects were too much. The dabrafenib-trametinib combo, once available, was the right choice since it targeted the BRAF mutation. That worked for some 20 months, so here we are now.
Will follow up with progress reports.

Dr. West, thank you for your feedback.

We hope to eventually generate some helpful and hopefully encouraging feedback. This being her fourth line of treatment means our options were limited.
Reflecting the first line of Carbo-Alimta (which you at the time you favored as well) worked for more than two years. The second line was docetaxel, which did work but she had to stop after seven courses because of the devastating side effects. This was in the atezolizumab trial OAK but she was assigned the docetaxel arm. The third line as the dabrafenib-trametinib combo which was possible because she had the BRAF V600E mutation. This worked for over a year and a half well in excess of the 9 months median.
We are grateful that we have had the good fortune to have workable options over the last six years and gope to add OPDIVO to that list.

Will post our experiences as they occur.

Dutch

UPDATE
After 6 courses nivolumab CT scan news showed: A more dense consolidation of 1.8x1.5 cm had resolved.

Worsening GGOs, inter/intralobular septal thickening and honeycombing, considered consistent with pulmonary interstitial fibrosis. May be post treatment change, malignancy not excluded.

Sscan was read off-site. My wife's oncologist and clinic's radiologist are inclined to consider this rather inflammatory than interstitial disease which would perhaps be a separate issue altogether.

if the dense consolidation had resolved, suggesting the nivolumab worked, can worsening GGO really be seen as malignant activity?

While not an accurate indicator, her CEA values had started to rise and was 3.5 last Feb, and now 1.2 the lowest since diagnosed 6-1/2 years ago when just below 9.

A mixed bag but malignant activity seems low. Confused abt a good aspect (consolidation gone-drug works) and perhaps not-so-good aspect (worsening GGOs-drug does not work)?

Anyone out there who has experienced this phenomena?

My wife, 70 yrs.
DX Mar 11 NSCLC mBAC (now called AIS).
Mar 11 lobectomy left LL & lower UL.
Scans: May 11 clean; July 11 bilateral GGOs; Sep 11 more prominent GGOs; Dec 11 worsening GGOs; Feb 12 PET scan further growth, no mets, BRAF positive (V600E);Mar 12 started Carbo-Alimta (6 courses) then Alimta maintenance; initial shrinkage then stable till early 2014; June 14 in trial MPDL3280A (atezolizumab) assigned docetaxel stopped Oct 14 side effects too severe. On chemo pause.
May 15 started Tafinlar-Mekinist. Feb 17 scan new growth. Treatment discontinued. Started nivolumab. Jun 17 scan Feb's new growth resolved, worsening GGOs, septal thickening and honeycombing.

Thanks Jim, your feedback much appreciated.
Dutch