Breast Cancer Clinical Trial
— ForesightOfficial title:
Foreseeing the Moments of Occurrence of Everolimus Long-term Side Effects by Follow up of Trough Blood Concentrations
Metastatic (HR-positive, HER2-negative) breast cancer (BC), advanced or unresectable
neuroendocrine tumours of pancreatic (pNET), gastrointestinal or lung origin and metastatic
renal cell carcinoma (mRCC) are diseases with poor outcome. Everolimus increases patients'
median progression-free survival (PFS) with 4.6 months in metastatic BC (mBC), 7 months in
(p)NET and 3 months in mRCC. However, serious adverse events (AEs) occur frequently. This
reduces effectiveness of everolimus, because AEs are managed with dose reductions, treatment
interruptions or even complete discontinuation of everolimus.
Therapeutic-drug-monitoring (TDM) is used to adjust the prescribed daily dose, to maintain
effective everolimus whole blood concentrations, with the lowest possible risk of AEs. While
everolimus TDM has been common in transplantation medicine, it has not been implemented in
oncology.
The importance of TDM in oncology is supported by previous research which showed that a
2-fold increased everolimus whole blood trough concentration was associated with a
short-term risk of grade ≥ 3 pneumonitis, stomatitis and metabolic events. Moreover, an
exposure-toxicity relationship of everolimus in patients with thyroid cancer was observed,
since initial everolimus concentrations could be associated with early toxicity (< 12 weeks,
e.g. stomatitis). However, the association between initial everolimus measurements and
long-term AEs (≥12 weeks, e.g. pneumonitis, anorexia and anemia) of any grade and the need
for everolimus dose reductions could not be made. Since levels ±>18 µg/L were associated
with toxicity, the investigators assume that the upper therapeutic window of everolimus in
the oncologic setting will be ±18 µg/L. Similarly, a tendency to improved PFS and overall
survival was observed when Cmin in steady state was above 14.1 μg/L. This seems to be the
lower limit of the therapeutic window.
Before consensus about the feasibility of everolimus TDM in the oncologic setting can be
achieved, a number of questions (the knowledge gaps) need to be answered: 1. It is unknown
whether everolimus whole blood trough levels (over time) predict long-term AEs. 2. The
optimal concentration range for everolimus, with the treatment of mBC, mRCC, or (p)NET is
unknown, especially the upper limit associated with toxicity. 3. It is unknown what
everolimus concentration level is associated with the need for everolimus dose reductions.
Status | Recruiting |
Enrollment | 40 |
Est. completion date | December 31, 2018 |
Est. primary completion date | September 1, 2018 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility |
Inclusion Criteria: - Patients currently treated with everolimus for any type of cancer, such as the EMA registered indications i.e. advanced (Hormone-Receptor [HR]-positive, HER2-negative) breast cancer, metastatic renal cell carcinoma (mRCC) or neuroendocrine tumour (NET) of pancreatic, gastrointestinal or lung origin. - Aged 18 or above - Able and willing to sign the informed consent Exclusion Criteria: - No informed consent - Alactasia |
Country | Name | City | State |
---|---|---|---|
Netherlands | Maastricht University Medical Centre | Maastricht | Limburg |
Lead Sponsor | Collaborator |
---|---|
Maastricht University Medical Center |
Netherlands,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Everolimus TDM to predict long-term toxicity | The difference in percentage of patients with a high everolimus trough level (i.e. > 18 ng/mL) experiencing NCI-CTCAE v4.0 grade 2, 3 or 4 late AEs (i.e. toxicity reported from = 12 weeks onward, e.g. pneumonitis, anorexia, anemia) compared to participants with lower trough concentrations. | Up to 2 year | |
Secondary | Everolimus TDM to predict short-term toxicity | The difference in percentage of patients with a high everolimus trough level (i.e. > 18 ng/mL) experiencing NCI-CTCAE v4.0 grade 2, 3 or 4 early AEs (i.e. toxicity reported from < 12 weeks, e.g. stomatitis) compared to participants with lower trough concentrations. | Up to 2 year | |
Secondary | Correlation everolimus concentration DBS from fingerprick with whole blood from venipuncture | To define the correlation between everolimus concentration measured in whole blood after a venipuncture as compared to the everolimus concentration measured from dried capillary blood extracted from the Whatman filterpaper of the DBS. | Up to 2 year | |
Secondary | Correlation everolimus concentration DBS from fingerprick with DBS spiked with whole blood from venipuncture | To define the correlation between everolimus concentration collected with DBS from a finger prick and DBS paper spiked with a drop of everolimus from venipunctured whole blood extracted from the Whatman filterpaper of the DBS. | Up to 2 year | |
Secondary | Everolimus TDM to predict dose reductions | To define the correlation between the everolimus trough levels (over time) between patients using full dose everolimus (e.g. 10 mg once daily) and patients using everolimus in a reduced dose (e.g. 2,5 or 5 mg once daily) at each moment of blood sampling in time. | Up to 2 year |
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