Aplidin filed for approval in myeloma in the EU
PharmaMar has filed for approval to market Aplidin to treat relapsed/refractory multiple myeloma in Europe, beating our expectation of a filing in Q4. The filing could potentially lead to approval in late H217 and market launch in late 2017 or early 2018. Aplidin has orphan drug designation in Europe and the US.
In March, the company announced positive top-line results from the 255-patient ADMYRE Phase III trial of Aplidin (plitidepsin) in relapsed/refractory multiple myeloma. The trial met its primary endpoint, showing a statistically significant 35% reduction in the risk of disease progression or death.
Multiple myeloma accounts for 10% of all haematological malignancies. It is caused by malignant plasma cells that multiply very rapidly. In 2015, 26,850 new cases were diagnosed in the US, and about 11,200 people died of this disease. In Europe, the incidence is 4.5-6.0 out of every 100,000 people each year.
Separately, in June the company initiated a pivotal Phase II trial of Aplidin for angioimmunoblastic T-cell lymphoma. We expect the initial approval for Aplidin in the US to be for this ultra-orphan indication, which accounts for 2% of non-Hodgkin’s lymphomas. The single-arm, open-label trial will recruit 60 patients from ~25 sites in Europe and the US; two sites were open at the end of July. Given the ultra-orphan nature of the disease we conservatively allow three years for the trial to complete and assume a US launch for Aplidin in H121. We expect Aplidin to reach global peak sales of US$300m, including US$115m in Europe.
PharmaMar has an Aplidin co-promotion agreement with Chugai Pharma Europe covering certain European countries (France, Germany, the UK, Benelux, Ireland and Austria). PharmaMar will earn a €4m milestone from Chugai for filing the marketing authorisation application to the European Medicines Agency.
Pharma Mar has also licensed marketing rights to Specialised Therapeutics Australia covering Australia, New Zealand and certain Asian countries, and to TTY Biopharm in Taiwan. It retains commercialisation rights in several key European territories, including Spain, Italy and Northern Europe, where we assume it will market Aplidin using its existing salesforce. PharmaMar also retains production rights and will supply Aplidin to its partners for sale in the licensed regions. There is potential for further licensing newsflow with Aplidin as the regulatory dossier for European approval will also be valid for more than 40 additional ex-EU countries.
PM1183: Ovarian clears interim futility, lung cancer underway
In August the CORAIL Phase III trial of PM1183 in ovarian cancer passed an interim futility analysis on the first 210 patients (50% of the total 420) and was cleared to continue recruiting. Recruitment is expected to complete around the end of 2016 with results likely in 2017. The CORAIL study is comparing PM1183 as a monotherapy in platinum-resistant ovarian cancer to a control arm with topotecan or liposomal doxorubicin. The primary endpoint is progression-free survival (PFS). This pivotal study follows encouraging PFS rates in a Phase IIb trial (Exhibit 3, below).
PharmaMar initiated a second pivotal study of PM1183 in August, this time in small cell lung cancer (SCLC). The ATLANTIS Phase III study builds on the impressive efficacy seen in a SCLC expansion cohort in a Phase Ib study. Preliminary results from the Phase Ib study showed that 67% of SCLC patients responded to PM1183 plus doxorubicin (including 10% complete responses), compared to response rates of 20-25% typically seen with standard-of-care drug topotecan. In patients who initially responded to first-line chemotherapy before relapse, the response rate was 100% (Exhibits 1 and 2).
ATLANTIS is a multicentre, open-label, randomised Phase III trial in 600 patients with relapsed (second-line) SCLC following platinum-containing therapy. The primary endpoint is progression free survival (PFS) comparing patients treated with the combination of PM1183 and doxorubicin to the control arm where patients are treated with either topotecan or a combination of cyclophosphamide, adriamycin and vincristine.
Exhibit 1: SCLC – maximum tumour size variation according to response to first-line chemotherapy
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Exhibit 2: SCLC – best confirmed response according to response to first-line chemotherapy
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Source: PharmaMar corporate presentation. Note: Sensitive = chemotherapy-free interval (CTFI) > 90 days after first line therapy; Resistant = CTFI ≤ 90 days; PD = progressive disease; PR = partial response.
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Source: PharmaMar. Note: CR = complete response; CTFI = chemotherapy-free interval; PD = progressive disease; PR = partial response; SD = stable disease.
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Exhibit 1: SCLC – maximum tumour size variation according to response to first-line chemotherapy
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Source: PharmaMar corporate presentation. Note: Sensitive = chemotherapy-free interval (CTFI) > 90 days after first line therapy; Resistant = CTFI ≤ 90 days; PD = progressive disease; PR = partial response.
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Exhibit 2: SCLC – best confirmed response according to response to first-line chemotherapy
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Source: PharmaMar. Note: CR = complete response; CTFI = chemotherapy-free interval; PD = progressive disease; PR = partial response; SD = stable disease.
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PM1183 is a synthetic alkaloid that is structurally related to PharmaMar’s drug Yondelis which is marketed for soft tissue sarcoma (STS) and platinum-sensitive ovarian cancer. However, PM1183 is being developed in different indications to Yondelis, including platinum-resistant ovarian cancer, SCLC, NSCLC and breast cancer. The compound has been optimised to improve the pharmacokinetic profile, such that PM1183 can be given at four times the tolerated dose level of Yondelis and offers administration advantages. PM1183 can be administered in a one-hour infusion using a peripheral intravenous catheter, compared to a 24-hour infusion with Yondelis via a central catheter.
Data are expected before the end of the year from a Phase II trial of PM1183 in metastatic breast cancer, which commenced in 2012. The primary endpoint of the 117-patient trial is overall response rate.
Exhibit 3: PM1183 (lurbinectedin) development status
Programme |
Indication |
Stage |
Notes |
PM1183 (lurbinectedin) |
Platinum-resistant/ refractory ovarian cancer (PRROC) |
Phase III |
420-pt monotherapy CORAIL trial in platinum-resistant ovarian cancer commenced recruitment in June 2015. The trial will compare PM1183 vs investigators’ choice of topotecan or pegylated liposomal doxorubicin (PLD). Recruitment is expected to complete in late 2016. In a Phase IIb trial PFS 5.7 months for PM1183 vs 1.7 months for topotecan (p=0.0005). Orphan drug status. |
Small cell lung cancer (SCLC) |
Phase III |
600-pt ATLANTIS trial as second-line therapy in combination with doxorubicin in platinum-resistant SCLC. Recruitment commenced August 2016, with final results due in 2019. The trial will compare PM1183 plus doxorubicin against either topotecan or a combination of cyclophosphamide, doxorubicin and vincristine. In a Phase I trial in 21 SCLC pts confirmed ORR was 67%, including 10% CR. |
BRCA1/2-associated breast cancer (BC) |
Phase II |
117-pt two-part Phase IIb trial in BRCA1/2-associated or unselected metastatic BC ongoing. Stage one: 20 pts with mut-BRCA1/2 mutation (targeting ≥ 4 pts with ORR) and 30 pts with unknown status (targeting ≥ 3 pts with ORR), leading into second stage with 33 pts in each arm if positive. Recruitment in the second stage is complete – results to be presented at ESMO in October. Primary endpoint ORR. |
Non-small cell lung cancer (NSCLC) |
Phase II |
120-pt three-arm Phase II of PM1183 ± gemcitabine vs docetaxel in second-line unresectable NSCLC. Primary endpoint: PFS at four months. Secondary endpoints: ORR, PFS/OS, histology. Phase I study + gemcitabine resulted in 1 CR, 4 PR and 7 SD in 19 evaluable NSCLC pts. |
“Basket” trial in advanced solid tumours |
Phase II |
225-pt Phase II of PM1183 in patients with advanced solid tumours, including SCLC, head and neck cancer, neuroendocrine tumours, biliary tract tumours, endometrial cancer, breast cancer, germ cell tumours and Ewing’s family of tumours. Primary endpoint: ORR. |
Source: Edison Investment Research, clinicaltrials.gov. Note: PFS = progression-free survival; IDMC = independent data monitoring committee; PTCL = peripheral T-cell lymphoma; ORR = overall response rate; CR = complete response; PR = partial response; SD = stable disease.
