IMMUNOTHERAPY FOR LOWER GASTROINTESTINAL CANCERS · PRINCIPLES OF IMMUNOTHERAPY. Chen et al. Clin...
Transcript of IMMUNOTHERAPY FOR LOWER GASTROINTESTINAL CANCERS · PRINCIPLES OF IMMUNOTHERAPY. Chen et al. Clin...
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IMMUNOTHERAPY FOR LOWER GASTROINTESTINAL CANCERS
Dr Elizabeth Smyth Cambridge University Hospitals NHS Foundation Trust
ESMO Colorectal Cancer Preceptorship Valencia 2019
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DISCLOSURES
Honoraria for advisory roleAstellas, Servier, Celgene, BMS, Five Prime Therapeutics, Gritstone Oncology
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OUTLINE
Immunotherapy primer
Colorectal cancer
Anal cancer
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PRINCIPLES OF IMMUNOTHERAPY
Chen et al. Clin Cancer Res 2012;
Antigen presentingCan cytotoxic T-cells be generated?
T-cell traffickingCan the T-cells get to the tumour?
Peptide-MHC recognitionCan the T-cells see the tumour?
PD-L1 on tumour/inhibitory cytokinesCan the T-cells be deactivated?
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BLOCKADE OF PD-1 OR CTLA-4 SIGNALING IN IMMUNOTHERAPY
Ribas A. NEJM 2012
Anti-CTLA4 antibodies (ipilimumab, tremilimumab)block a negative regulatory signal during T-cell priming.
Anti-PD-1 antibodies (pembrolizumab, nivolumab) blockthe negative regulatory signal of PD-1 which isexpressed on T-cells during long term antigenexposure.
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I. COLORECTAL CANCER
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POLE mut
MSI-HLow mutation burden
Grasso et al, Cancer Discovery 2018
Immune checkpoint blockade efficacy
COLORECTAL CANCER MOLECULAR LANDSCAPEIn CRC high mutation burden = IO efficacy
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COLORECTAL CANCER AND IMMUNOTHERAPY MMRd vs MMRp tumours
From an immunotherapy perspective there are two CRC categories1. Mismatch repair deficient (MMRd) – 2-5% of Stage IV cancers, more common in Stage II>III2. Mismatch repair proficient (MMRp) - majority of Stage IV cancers
Mismatch repair status can be assessed using:• Protein immunohistochemistry for MMR proteins (MLH1, MSH2, MSH6 and PMS2)
PCR to detect high levels of microsatellites in DNA (microsatellite instablilty, MSI)Next generation sequencing
>80% of MMRd tumours are sporadic (methylation of MLH1), however as 15-20% may be germline (Lynch syndrome) genetics referral should be considered in MMRd patients.
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MISMATCH REPAIR DEFICIENCY AND THE IMMUNE SYSTEM
Baretti et al, Pharmacol Ther. 2018
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PEMBROLIZUMAB IN MMRD AND MMRP CRC MMRP or MMRD (loss of MLH1, MSH2, MSH6 or PMS2 , or MSI in ≥ 2 loci) ≥ 2 prior cancer therapy regimens ECOG PS ≤ 1
Outcome MMRD CRC(n = 28)
MMRP CRC(n = 25)
Overall response rate, % 57 0 Response, % CR PR SD PD Not evaluable
11463247
00164440
Median PFS, mos NR 2.3Median OS, mos NR 6.0
Le DT, et al. ASCO 2016. Abstract 103Le DT et al, NEJM 2015
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PEMBROLIZUMAB IN MMRD/MMRP CRCDeep and sustained responses in MMRd patients treated with pembrolizumab
Le DT, et al. ASCO 2016. Abstract 103.
May 2017 – FDA licensed pembrolizumab in previously treated MMRD colorectal cancer
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PEMBROLIZUMAB IN MMRD/MMRP CRCKEYNOTE 164
Le DT, et al. ESMO World GI 2018
Responses observed in all lines of therapy
ORR 32%
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PEMBROLIZUMAB IN MMRD/MMRP CRCKEYNOTE 142 long term follow up
Le DT, et al. ESMO World GI.
Benefits of anti-PD-1 therapy are sustained in MMRd CRC76% alive at one year follow up
Le DT, et al. ESMO World GI 2018
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NIVOLUMAB FOR MMRD-CRCCHECKMATE-142
Overman et al Lanet Oncol 2017
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NIVOLUMAB FOR MMRD-CRCCHECKMATE-142
Benefits of nivolumab in MMRD CRC very similar to those observed for pembrolizumab
ORR 34%
Overman, Lancet Oncol 2017
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BENEFIT INDEPENDENT OF PD-L1, BRAF OR LYNCH STATUS
Overman, Lancet Oncol 2017
Anti-PD1 therapy is a good choice for MMRd patients regardless of family history, BRAF status or PD-L1 expression
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NIVOLUMAB FOR MMRD-CRCCHECKMATE-142
Median OS not reached12 month OS 68% (A) vs 81%(B)
Median PFS 6.6 monthsMedian PFS 4.2m (A) vs NR(B)
August 2017 – FDA licensed nivolumab in MMRD colon cancers
48% progression free and 74% alive at 1 year
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NIVOLUMAB FOR MMRD-CRCCHECKMATE-142
Overman et al, ASCO GI 2018
No responding patient relapsed during follow up
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LICENSING STATUS OF ANTI-PD-1 THERAPIES
• Neither pembrolizumab nor nivolumab is licensed by EMA for treatment of MMRd colorectal cancer
• Randomised data are awaited
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NIVOLUMAB + IPILIMUMAB FOR MMRD-CRCCHECKMATE-142
Overman et al, JCO 2018
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NIVOLUMAB + IPILIMUMAB FOR MSI-CRCInvestigator assessed response
Andre et al, ASCO GI 2018Overman et al, Journal of Clinical Oncology 2018
ORR to combination therapy appears greater than nivolumab alone (no formal comparison planned)
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NIVOLUMAB + IPILIMUMAB FOR MSI-CRCProgression free and overall survival
Andre et al, ASCO GI 2018Overman et al, Journal of Clinical Oncology 2018
Combination nivolumab/ipilimumab results in 71% 12 month progression free survival and 85% one year overall survival
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NIVOLUMAB + IPILIMUMAB FOR MSI-CRCSafety data
Toxicity with combination ipilimumab plus nivolumab
10% patients discontinued treatment
Andre et al, ASCO GI 2018Overman et al, Journal of Clinical Oncology 2018
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MOVING IMMUNOTHERAPY INTO EARLIER LINESCHECKMATE 142 1L cohort
Lenz et al, ESMO 2018
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NIVOLUMAB AND IPILIMUMUAB IN 1LCHECKMATE 142 1L cohort
ORR 60%
Lenz et al, ESMO 2018
ORR not compromised by low dose ipilimumab
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NIVOLUMAB AND IPILIMUMUAB IN 1LCHECKMATE 142 1L cohort
Lenz et al, ESMO 2018
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TOXICITY IS IMPROVED WITH LOW DOSE IPILIMUMAB
Nivolumab plus low dose ipilimumab is a safe and effective choice for MMRd CRC (not yet licensed)
Nivo + q3wk ipi Nivo + q6wk ipiGrade 3-4 TRAE 32% 16%Serious TRAE 20% 7%Discontinuation 10% 2%
Lenz et al, ESMO 2018
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NEOADJUVANT IMMUNOTHERAPY FOR MMRD CRCNeoadjuvant nivolumab plus ipilimumab: NICHE study
Chalabi et al, ESMO 2018
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NEOADJUVANT IMMUNOTHERAPY FOR MMRD CRCNeoadjuvant nivolumab plus ipilimumab
Chalabi et al, ESMO 2018
No residual tumour in MMRd patients treated with nivolumab plus ipilimumab
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NEOADJUVANT IMMUNOTHERAPY FOR MMRD CRCNeoadjuvant nivolumab plus ipilimumab
Chalabi et al, ESMO 2018No/minimal effect of MMRp patients treated with nivolumab plus ipilimumab
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Neither pre-treatment CD3 infiltrate nor immune gene signature were predictive of response to nivo/ipi
NEOADJUVANT IMMUNOTHERAPY FOR MMRD CRCNeoadjuvant nivolumab plus ipilimumab
Chalabi et al, ESMO 2018
Pre-treatment CD3 Pre-treatment gene signature
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BIOMARKERS IN MMRD CRCDoes tumour mutation burden matter?
High TMB was associated with higher change of radiological response, and improved PFS and OSCaveat – small dataset (n=22), targeted panel to assess TMB
Shrock et al, Annals Oncol 2019
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BIOMARKERS IN MMRD CRCMarkers of resistance and secondary targets
• Recurrent mutations and LOH in antigen presenting machinery (HLA, B2M) in MSI tumours
• JAK1/2 mutations
Grasso et al, Cancer Discovery 2018Shin et al, Cancer Discover 2016
Pietrantonio et al, JCNI 2017Bass, Nature 2109
• High incidence of TRK, ALK, ROS fusions – consider referring for screening for clinical trials
• Synthetic lethality with Werner helicase inhibition
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IMMUNOTHERAPY FOR MMRD CRCConclusions
• Anti-PD-1 is a standard of care for MMRD CRC associated with high response rates and durable benefit
• European license awaited pending randomised data
• Dual immunotherapy blockade will become standard, low dose ipilimumab appears safe and tolerable
• Moving immune checkpoint blockade to earlier lines of therapy is an exciting prospect
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IMMUNOTHERAPY FOR MMRP CRC
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CHECKPOINT IMMUNE BLOCKADE IS INEFFECTIVE IN MSS CRC
Author Drug N ORRLe et al MSS CRC Pembrolizumab 18 0%Overman et al MSS CRC Nivolumab + ipilimumab 20 5%Chung et al Refractory CRC Tremelimumab 49 2%Topialan et al Refractory CRC Nivolumab 19 0%
Lee et al, N. Engl. J. Med. 2015;372:2509–2520Overman et al, J. Clin. Oncol. 2016;34:3501.
Chung et al, J Clin Oncol. 2010 Jul 20; 28(21):3485-90.Topialian et al, N. Engl. J. Med. 2012;366:2443–2454. doi: 10.1056/NEJMoa1200690.
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COLORECTAL CANCER MOLECULAR AND IMMUNE LANDSCAPE
Gunney et al, Nat Med. 2015 Nov;21(11):1350-6 Dientsmann et al, Nature Reviews Cancer volume 17, pages 79–92 (2017)
Becht et al, Clin. Cancer Res. 2016;22:4057–4066. .
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CMS2, WNT ACTIVATION AND IMMUNE EVASION
Guiney et al, Nat Med. 2015 Nov;21(11):1350-6 Grasso et al, Cancer Discovery 2018
CRC TCGA, Nature 2012
Most current WNT inhibitors are upstream of APC mutation
High beta-catenin expression results in low CD3 and CD8 infiltrate
T-cell average vs AXIN2 expression APC mt, AXIN and T cell infiltrate
WNT signalling via APC mutation is fundamental in CRC
Targeting WNT is challenging! Most inhibitors are upstream of APC; exception porcupine inhibitors
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CMS3, MAPK SIGNALLING AND IMMUNE EVASION
Guiney et al, Nat Med. 2015Ebert PJ, et al. Immunity. 2016
Bendell J, et al. ASCO 2016. Abstract 3502 CRC TCGA, Nature 2012
In preclinical models, inhibition of MEK signalling leads to ↑ CD8 T cell infiltration and MHC1 expression Combinatoin of MEKi and anti-PD-L1 showed synergy
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TARGETING MAPK AND IMMUNE IN CRCCobemetanib plus atezolizumab in mCRC
Bendell et al, ASCO GI 2018
Early results were positive
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TARGETING MAPK AND IMMUNE IN CRCCobemetanib plus atezolizumab in mCRC: IMBLAZE
Bendell et al, Lancet Oncol 2019
ORR <3% in all armsNo difference in PFS or OS
Outcome not different in RAS mt patients
Future questionsScheduling of MEKi – effect on T-cells
MEK signaturesNovel IO combinations
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Role for CXCR3TARGETING MAPK AND IMMUNE IN CRC
• KRAS mutation decreases IRF2 expression • Decreased IRF2 leads to increased CXCL3 expression• CXCL3 acts on CXCR2 on MDSC to attract to TME• MDSC causes immunosuppression
• In mouse models, inhibition of CXCR2 leads to increased sensitivity to immunotherapy
Liao et al, Cancer Cell 2019
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1 CRC responder:MSS, CMS4, KRAS mutant and PD-L1+, high signature for complement cascade and MDSC
TARGETING TGF-B IN CMS 4 CRC
M7824Bifunctional fusion protein targeting PD-L1 and TGF-β
Lan et al, Sci Trans Med 2018Kopetz et al, ASCO GI 2018
Ongoing clinical trial in CMS4 CRC
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TGF-Β INDUCTION BY RADIOTHERAPY AS TARGET FOR IMMUNOTHERAPY COMBINATIONS
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BEST RT DOSE QUESTION
Vanpouille-Box et al, Nature Comm 2017,
RADIOTHERAPY DOSE AND IMMUNE RESPONSE
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ANGIOGENESIS AS A MECHANISM OF IMMUNE EXCLUSIONMODUL BRAFwt cohort
Grothey et al, ESMO 2018
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ANGIOGENESIS AS A MECHANISM OF IMMUNE EXCLUSION
Grothey et al, ESMO 2018MODUL results: no benefit to addition of anti-PD-L1 to FP-bev in MSS
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ANGIOGENESIS AS A MECHANISM OF IMMUNE EXCLUSIONAnti-angiogenic TKI +IO in other cancers
HCC H&N
Endometrial
Breaking newsASCO 2019
Fukuoka et al abstract 2552Regorafenib + nivolumab
MSS CRC cohort 29% ORR
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Tabernero et al, ASCO 2017
BRINGING THE T CELLS TO THE TUMOUR: CEA BISPECIFIC
ORR 6% ORR 18%
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IS THERE HOPE FOR MSS CRC?
Chen et al, ASCO GI 2019
Concerns1. Extra interventions in experimental arm
2. High alpha 0.1 risks false positive 3. No PFS correlate for OS benefit
4. No responses in experimental arm
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IMMUNOTHERAPY IN MMRP COLORECTAL CANCER
• Multiple mechanisms lead to immune evasion in MMRp CRC including WNT, MAPK, and TGFβ signalling
• WNT signalling is difficult to target due to upstream site of APC mutation, downstream inhibitors are required
• Targeting MAPK signalling has not been successful in increasing sensitivity to immunotherapy
• Targeting TGFβ shows promise in early phase trials for CMS4 patients
• CEA bispecifc antibody plus immunotherapy also shows early evidence of activity
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II. ANAL CANCER
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RATIONALE FOR IMMUNOTHERAPY IN ANAL CANCER
Martin et al, Biochimica et Biophysica Acta 2017
90% HPV positive
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NIVOLUMAB IN ANAL CANCERFirst evidence of efficacy of anti-PD1 in anal cancer
PD-L1 unselectedORR 24%
Median PFS 4.1 months Median OS 11·5 months
Morris et alm Lancet Incol 2017
Increased ORR in high CD8 and PDL1Small numbers”
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PEMBROLIZUMAB IN ANAL CARCINOMAKEYNOTE 028
All patients were PD-L1 positive (74% of screened)Mostly pretreated
ORR 17% (4/24 SCC patients)
Median PFS 3.5 months (95% CI 1.7–7.3 months)Median OS 9.3 months (95% CI, 5.9 months
to not reached)
Ott et al, Annals Oncol 2017
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ANAL CANCER BIOMARKERSHPV ctDNA as a prognostic and response metric
HPV ctDNA under anti-PD-1 therapy
Bernard-Tessier et al, CCR 2019Cabel et al, IJC 2017
HPV ctDNA after chemotherapy is prognostic
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ANAL CANCER AND IMMUNOTHERAPYSummary
• Anal carcinoma is a virally driven, immunogenic tumour • Preliminary results in previously treated patients are encouraging• Randomised data and integration into earlier lines of therapy are awaited