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Ronny Allan
"Interestingly, the ORR in pancreatic NETs was 44%, a rate not seen before with targeted agents,"
Lenvatinib has completed a Phase 2 trial in Gastrointestinal (GI) and Pancreatic Neuroendocrine Tumours. The trial was sponsored by Grupo Espanol de Tumores Neuroendocrinos (Spanish NET scientific organisation) and the manufacturers. A European venture with sites in Austria, Italy, Spain, UK. Headline: The responses are better than Everolimus (Afinitor) and Sunitinib (Sutent).
What is Lenvatinib?
It is a type of targeted therapy known as a multikinase inhibitor. The brand name is ‘LENVIMA‘. These work by inhibiting multiple intracellular and cell surface kinases, some of which are implicated in tumour growth and metastatic progression of cancer, thus decreasing tumour growth and replication. A range of receptor kinases is involved in these processes, including vascular endothelial growth factor receptor (VEGFR), platelet-derived growth factor receptor (PDGFR), stem cell factor (c-KIT), Flt3, fibroblast growth factor receptor (FGFR), which can be hyperactivated during tumour formation and progression. Tumour growth may be prevented by inhibiting the action of these hyperactivated receptor kinases, and as tumour progression usually involves the action of multiple kinases rather than just one, it is logical to target multiple kinases.
The Lenvantinib mechanism of action is similar to targeted therapy drugs already in use (or in trial) for Neuroendocrine Tumours:
- Sunitinib (Sutent) – a targeted therapy receptor protein-tyrosine kinase inhibitor. It inhibits the actions of vascular endothelial growth factor (VEGF) and is an angiogenesis inhibitor (i.e. the development of blood vessels to supply the tumour with nutrients, which they need to grow). It is a mutlikinase in inhibitor. Click here
- Everolimus (Afinitor) – a targeted therapy kinase inhibitor that inhibits mammalian target of rapamycin (mTor) kinase, an enzyme required for cell growth and survival. By blocking this enzyme, the medication prevents cell division and, in turn, tumor growth. The medication can also interrupt angiogenesis. Click here
- Cabozantinib, an oral potent inhibitor of vascular endothelial growth factor receptor 2, MET, and AXL, and currently on trial for Neuroendocrine Cancer. Click here.
Multikinase inhibitors such as Lenvatinib, may be used to treat advanced kidney cancer as well as other specific types of cancer (in my research I also noted that in addition to kidney cancer, the drug is already approved for liver and thyroid cancers). Worth also noting that the 3 examples of targeted therapy above are not just in use/in trial for Neuroendocrine Cancer, they are also in use/in trial for others including Renal (Kidney) Cancer, Breast Cancer. Often more than one single kinase inhibitor can be given as a combo treatment, perhaps in sequence, to tackle multi kinases.
In this multicenter, open-label study involving 111 patients, treatment with lenvatinib (Lenvima) led to an overall response rate (ORR) of 29.9%, with a particularly high ORR — 44.2% — in patients with pancreatic NETs, reported Jaume Capdevila, MD, PhD, of Vall Hebron University Hospital in Barcelona, and colleagues.
Worth noting that Everolimus and Sunitinib were approved with ORRs much less than these figures.
Lenvatinib showed significant antitumor activity and a favourable toxicity profile in progressive advanced NETs. This is the highest reported ORR with a targeted agent, confirmed by central radiology assessment in pancreatic NETs and Gastrointestinal (GI) NETs with promising progression-free survival (PFS) in a pre-treated population; further evaluation is warranted.
Adverse events were mild to moderate in 90% of patients, the most frequent being fatigue, diarrhea and hypertension.
The Results of the Phase 2 Trial
The results were published – click here (but see abstract below).
Abstract
Purpose: Approved systemic therapies for advanced gastroenteropancreatic neuroendocrine tumors (GEP-NETs) have shown limited capacity to reduce tumor burden and no antitumor activity after progression to targeted agents (TAs). We investigated the efficacy and safety of lenvatinib in patients with previously treated advanced GEP-NETs. Patients and methods: This was a multicenter, single-arm, open-label, phase II trial with two parallel cohorts (ClinicalTrials.gov identifier: NCT02678780) involving 21 institutions in 4 European countries. Eligible patients had histologically confirmed advanced grade 1-2 pancreatic (panNET) or GI (GI-NET) NETs with documented tumor progression after treatment with a TA (panNET) or somatostatin analogs (GI-NET). Patients were treated with lenvatinib 24 mg once daily until disease progression or treatment intolerance. The primary end point was overall response rate by central radiology review. Secondary end points included progression-free survival, overall survival, duration of response, and safety. Results: Between September 2015 and March 2017, a total of 111 patients were enrolled, with 55 (panNET) and 56 (GI-NET) patients in each cohort. The median follow-up was 23 months. The overall response rate was 29.9% (95% CI, 21.6 to 39.6): 44.2% (panNET) and 16.4% (GI-NET). The median (range) duration of response was 19.9 (8.4-30.8) and 33.9 (10.6-38.3) months in the panNET and GI-NET groups, respectively. The median progression-free survival was 15.7 months (95% CI, 14.1 to 19.5). The most common adverse events were fatigue, hypertension, and diarrhea; 93.7% of patients required dose reductions or interruptions. Conclusion: We report the highest centrally confirmed response reported to date with a multikinase inhibitor in advanced GEP-NETs, with a particularly strong response in the panNET cohort. This study provides novel evidence for the efficacy of lenvatinib in patients with disease progression following treatment with other TAs, suggesting the potential value of lenvatinib in the treatment of advanced GEP-NETs.
Capdevila, Jaume & Fazio, Nicola & López, Carlos & Teule, A. & Valle, Juan & Tafuto, Salvatore & Custodio, Ana & Reed, Nicholas & Raderer, Markus & Grande, Enrique & Garcia-Carbonero, Rocio & Fonseca, Paula & Hernando, Jorge & Bongiovanni, Alberto & Spada, Francesca & Alonso, Vicente & Antonuzzo, Lorenzo & Spallanzani, Andrea & Berruti, Alfredo & Ibrahim, Toni. (2021). Lenvatinib in Patients With Advanced Grade 1/2 Pancreatic and Gastrointestinal Neuroendocrine Tumors: Results of the Phase II TALENT Trial (GETNE1509). Journal of clinical oncology : official journal of the American Society of Clinical Oncology. 39. JCO2003368. 10.1200/JCO.20.03368.
What’s next?
Given the responses in comparison to other approved targeted agents, a phase 3 trial should be anticipated. Studies are “currently ongoing” and “further evaluation warranted”.
I will keep this article live to provide updates. As at 27 February 2024, no news of Phase 3 trial.
Finally
Whenever I post about a trial or study, some people get excited without understanding that these new treatments and capabilities can very often take years to come to fruition and it’s also possible that clinical trials can be halted, or that national approval agencies will not approve the final product. Plus, not everyone will be eligible, so always check the exclusion and inclusion criteria in the relevant clinical trials document. Please bear that in mind when reading studies/clinical trials posted on RonnyAllan.NET
Other clinical trials
Clinical Trial using Lenvatinib and Everolimus in Treating Patients With Advanced, Unresectable Neuroendocrine Tumors
Under ClinicalTrials.gov Identifier: NCT03950609, there is a phase 2 trial running at MD Anderson in Texas USA (estimated completion 20 Jun 2024). Use of a combo of Lenvatinib along with Everolimus (Afinitor) in treating patients with advanced, unresectable Neuroendocrine Tumors (sorry the word ‘Carcinoid‘ is used in the trial documentation).
Clinical Trial using Lenvatinib and Keytruda in Treating Patients With Advanced, Unresectable Neuroendocrine Tumors
ClinicalTrials.gov Identifier: NCT03290079. a trial run by Moffatt Tampa. As of 3rd Aug 2022, the recruiting was suspended pending interim results analysis. Trial will not progress further noting “Neither sufficient shrinkage to qualify for PR nor sufficient increase to qualify for Progressive Disease”
Clinical Trial for Pheo/Para
ClinicalTrials.gov Identifier: NCT03950609. Based out of May Rochester. Only 3 participants took park. Study completed 2022-09-28. No results posted. Outcome not known from clinical trial record linked above.
Reference material used in the compilation of this article:
1. Annals of Oncology – Efficacy of Lenvatinib in patients with advanced pancreatic (panNETs) and gastrointestinal (giNETs) grade 1/2 (G1/G2) neuroendocrine tumors: Results of the international phase II TALENT trial (GETNE 1509) 23 Oct 2018 – click here.
2. ESMO Congress 2018 – Efficacy of Lenvatinib in patients with advanced pancreatic (panNETs) and gastrointestinal (giNETs) grade 1/2 (G1/G2) neuroendocrine tumors – click here
3. Prime Oncology Slide Show – click here (useful)
4. TALENT Clinical Trials Document NCT02678780 – click here
5. Manufacturer’s website – click here.
6. Clinical Trials Document NCT03950609 for the trial of combo treatment Lenvatinib and Everolimus. Click here. As at 15 May 2019, the trial was not recruiting but see the document for contact details, quite often these documents can be behind in updating. Trial start date is recorded as 30 June 2019.
7. ClinicalTrials.gov Identifier: NCT03950609. For Pheo/Para.
8. ClinicalTrials.gov Identifier: NCT03290079. Lenvatinib with Keytruda
9. ASCO Journal of Clinical Oncology DOI: 10.1200/JCO.20.03368 Journal of Clinical Oncology published online May 04, 2021.
Disclaimer
I am not a doctor or any form of medical professional, practitioner or counsellor. None of the information on my website, or linked to my website(s), or conveyed by me on any social media or presentation, should be interpreted as medical advice given or advised by me.
Neither should any post or comment made by a follower or member of my private group be assumed to be medical advice, even if that person is a healthcare professional.
Please also note that mention of a clinical service, trial/study or therapy does not constitute an endorsement of that service, trial/study or therapy by Ronny Allan, the information is provided for education and awareness purposes and/or related to Ronny Allan’s own patient experience. This element of the disclaimer includes any complementary medicine, non-prescription over the counter drugs and supplements such as vitamins and minerals.
General Clinical Trials Disclaimer
Choosing to participate in a study is an important personal decision. Talk with your doctor and family members or friends about deciding to join a study. To learn more about this study, you or your doctor may contact the study research staff using the contacts provided in the clinical trials document. It’s very important to check the trial inclusion and exclusion criteria before making any contact. If you need questions, the articles here is very useful Questions to Ask About Clinical Trials | Cancer.Net
The inclusion of any trial within this blog should not be taken as a recommendation by Ronny Allan.
Finally
Whenever I post about a trial or study, some people get excited without understanding that these new treatments and capabilities can very often take years to come to fruition and it’s also possible that clinical trials can be halted, or that national approval agencies will not approve the final product. Plus, not everyone will be eligible, so always check the exclusion and inclusion criteria in the relevant clinical trials document. Please bear that in mind when reading studies/clinical trials posted on RonnyAllan.NET
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Hi, there. This is straight from the horse’s mouth: I was part of the Spain Lenvatinib trial from May 2016 to end of October 2017 (I live in Madrid). Having been diagnosed with and had surgery for locally advanced pancreatic neuroendocrince cancer in 2011, I experienced PFS till late 2015 when the beast came back in the form of liver metastasis. A first clinical trial did not work and I entered the Lenvatinib trial. I was put on the full 24 mg dose initially but this was gradually reduced and I was on the minimum 10mg by the time I exited the trial in 2017. I left as my tolerance to the toxicity had reached its limit and I could not continue with the nausea, diarrea, severe joint and muscular pain. I should add that I am very sensitive to medication. Over the 18 months I was on the trial, the cancer spots on my liver shrank considerably and my CgA levels are today almost within normal range. (I take PPIs which can skew results). I was also treated with SBRT. Since then, I have been put on Somatuline Autogel 120 and I have 3-monthly CT scans, with an Octreoscan SPECT/CT scan before Christmas. Nearly 15 months after coming off Lenvatinib I show no tumoral activity. Needless to say, I hold my breath between scans (next one in March) but know that awareness of neuroendocrine cancer has grown enormously since my initial diagnosis – thanks in part to blogs such as Ronny’s – and that this impacts research. Sad deaths such as Aretha Franklin’s also help to strengthen awareness. My oncologist tells me that should I have a relapse, then he’ll recommend PRRT. I am blessed to live in a part of the world where all this is a) available and b) available through the public health system.
Good luck to one and all and unending thanks to Ronny for keeping us up to date.
There is so much hope now in this sneaky cancer . I just want to live and live …life is so wonderful…now there is even more hope and time for us n e t s people!! Just a shame sometimes we have to shout out for it! My doctor recently scared me by calling after a 5 1ahh sample saying it was high again…I immediately brought my consultant appointment forward and worried constantly for the weeks wait….only to be told it was actually LOWER than ever before and I can now after 2 and a bit years go to 6 monthly appoint….jumping for joy was an understatement!!!
Keep it up Ronnie….you are doing a great job in reporting the latest and greatest. Liver Mets continues as the most irritating but treatable in different stages. We need more and more on this topic! Thank You!