Cholangiocarcinoma Clinical Trial
Official title:
A Phase 2A, Single Arm, Multicentre, Study of ASLAN001 in Patients With Advanced or Metastatic Cholangiocarcinoma Who Progressed on at Least 1 Line of Systemic Therapy
This is a single arm, multicentre, Phase 2 study to assess efficacy and safety of ASLAN001 in
patients with advanced or metastatic cholangiocarcinoma who progressed on at least 1 line of
systemic therapy.
25 evaluable patients will be enrolled in the study. After evaluation of initial response in
the first 10 evaluable patients, Sponsor will make a decision on recruitment of an additional
15 evaluable patients. If no response is observed, the study will stop.
The primary objective is to assess efficacy of varlitinib (also known as ASLAN001) as
measured by ORR (based on RECIST v1.1). The secondary objectives are to (1) evaluate the
efficacy of varlitinib, as measured by DoR, PFS, OS and DCR, (2) assess ORR, DoR, PFS, DCR
and OS by tumor EGFR/HER2 status, (3) assess safety and tolerability of ASLAN001 monotherapy.
Exploratory objectives are to explore possible relationships between response to ASLAN001 and
the protein expression levels and gene mutational status of the proteins and genes via IHC
and PCR/Sequencing.
Cholangiocarcinoma (CCA) is a malignancy arising from the biliary epithelium characterized by
poor prognosis and poor response to current treatments. Emerging at any portion of the
biliary tree, it includes a group of tumours with epidemiologic, morphologic, biologic, and
clinical heterogeneity. Despite recent medical advances, the long-term outcomes and
recurrence rates for CCA are poor. The 5-year survival rate following surgical resection is
11-40%. Tumour recurrence rates are as high as 50-65%, with a median time to recurrence
between 12-43 months.
In the United States, the incidence and mortality of CCA have increased over the last 30
years without clear underlying etiological reasons. The only curative therapy is surgical;
however this is not an option for many patients given the stage of the disease at
presentation and metastasis. While improvements in diagnostic modalities and neoadjuvant
chemotherapy have allowed for detection at earlier stages and greater survival rates, the
prognosis is still unfavorable. Therapies that can decrease tumour growth, improve resection
outcomes, increase survival rates, and decrease recurrence would make a great impact on the
quality of life of CCA patients and are urgently needed.
Currently, the Food and Drug Administration (FDA)-approved agents used in unresectable CCA
include gemcitabine, capecitabine, cisplatin, oxaliplatin, fluoropyrimidines (including
5-fluorouracil), or a combination of these. However, none are FDA-approved primarily for use
in CCA specifically. Gemcitabine and cisplatin combination therapy, along with
fluoropyrimidine-based or other gemcitabine-based regimens are part of the guidelines for
unresectable cancer per the National Comprehensive Cancer Network. To date, the most
effective chemotherapy regimen is administration of gemcitabine with cisplatin or
oxaliplatin, which have now become the standard of care for systemic therapy. Even this most
efficacious treatment has been found to only modestly increase overall survival (11.7 months
vs 8.3 months for patients receiving gemcitabine alone) and progression-free survival (8.4 vs
6.5 months). Standard treatment as second-line chemotherapy for CCA is unclear as there is no
significant evidence for specific therapy which indicates that further chemotherapy beyond
progression on first-line chemotherapy improves survival.
CCA involves mutations in members of the ErbB family, including EGFR and HER2 mutations. EGFR
is overexpressed in both intrahepatic and extrahepatic CCA (30.8% and 20.9%, respectively)
and is an independent prognostic factor in intrahepatic cases, per Yang et al 2014. While
this study found overexpression of HER2 exclusively in extrahepatic samples (and only in 4.5%
of these), previous studies have implicated this protein in both extra- and intrahepatic
tumours. Settakorn et al (2005) showed HER2 expression is correlated with high histological
grade in intrahepatic CCA. Kim et al. (2007) found HER2 (gene and protein levels) are
overexpressed in approximately 30% of extrahepatic CCA patients and is a prognostic factor
for survival in those with lymph node metastasis.
EGFR, HER2, and HER4 are single-pass transmembrane glycoprotein receptors, members of the
type I receptor tyrosine kinase family. Upon ligand binding, their activation induces the
homo- or heterodimerization and subsequent phosphorylation of intracellular tyrosines, which
lead to both cell proliferation and survival and therefore cancer development and
progression. EGFR and HER2 inhibitors have both demonstrated clinical efficacy in cancer
treatment. The simultaneous inhibition of both represents a new therapeutic approach for
broadly targeting different tumour types that may be more effective than selective inhibition
of each receptor.
Varlitinib, also known as ASLAN001 is a potent, orally active inhibitor of the receptor
tyrosine kinases epidermal growth factor (EGFR) and human epidermal growth factor receptors 2
and 4 (HER2, HER4). In cell-based assays, varlitinib has been shown to potently inhibit the
phosphorylation of EGFR, HER2, and HER4 in a dose-dependent manner. In cell lines
overexpressing HER2, varlitinib also inhibited the phosphorylation of the HER2 downstream
effector AKT.
ASLAN hypothesises that varlitinib will inhibit EGFR, HER2, HER4 as their mutations results
in CCA, thus in turn inhibiting the growth of cancerous cells and development/progression.
ASLAN believes that varlitinib is a compound that may be beneficial to patients with cancer
by simultaneous inhibition of these receptors.
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