Healthy Volunteers Clinical Trial
Official title:
A Phase 1 Open-label, Radiolabeled, Single-dose Study To Investigate The Metabolism Of [14c]Lorlatinib (Pf-06463922) In Healthy Male Volunteers
This open-label, radiolabeled, single 100-mg dose study in 6 healthy male volunteers has been
designed to further the understanding of human metabolism of lorlatinib. A prior radiolabel
study using [14C]lorlatinib (study B7461004) identified an unexpected major metabolite in
plasma; a benzoic acid metabolite (M8) resulting from cleavage of the amide and aromatic
ether bonds of lorlatinib, accounting for 21.0% of the circulating radioactivity. However,
due to the position of the 14C radiolabel on the carbonyl carbon, the metabolic fate of the
larger fragment of lorlatinib resulting from this cleavage, the pyrido-pyrazole substructure,
could not be determined. In this current study, the radiolabel will be on the pyrazole ring
allowing for monitoring the metabolic fate of the pyrido-pyrazole part of the lorlatinib
molecule cleaved during the formation of the M8 metabolite. Since M8 will not be
radiolabeled, its concentrations in plasma will be determined using a validated assay.
The sample size of 6 was selected to ensure at least 4 fully evaluable subjects with
completed collections of plasma, urine, and fecal samples. This is a standard sample size
used for mass-balance/ADME studies which include assessment of metabolic profiling, and is
not based on empirical data or hypothesis testing criteria.
Metabolic profiling of radiolabeled components will be performed on pooled plasma samples as
well as on cumulative urine and feces excreted until Day 14 postdose or until one of the
following early release criteria is met: 1) recovery in excreta of at least 90% of
administered radioactivity, or 2) less than 1% of administered radioactivity being recovered
in excreta from two consecutive days (ie, total for urine + feces should be <1% on 2
consecutive days). Plasma concentrations of both lorlatinib and its unlabeled M8 metabolite
will be analyzed using validated assays. Information from this study will complement the
metabolic profiling results from study B7461004, will help guide in the assessment of
potential drug-drug interactions (DDIs) and the need for other DDI studies with lorlatinib.
Banked biospecimens will be collected for the purpose of conducting research. Collecting
biospecimens for exploratory analyses makes it possible to better understand the
investigational product's mechanism of action and to seek explanations for differences in,
for example, exposure, tolerability, safety, and/or efficacy not anticipated prior to the
beginning of the study.
This open-label, radiolabeled, single 100-mg dose study in approximately 6 healthy male
volunteers has been designed to further the understanding of human metabolism of lorlatinib.
A prior radiolabel study using [14C]lorlatinib (study B7461004) identified an unexpected
major metabolite in plasma; a benzoic acid metabolite (M8, PF-06895751) resulting from
cleavage of the amide and aromatic ether bonds of lorlatinib, accounting for 21.0% of the
circulating radioactivity or ~ 47.3% plasma M8 to lorlatinib AUC percent ratio. However, due
to the position of the 14C radiolabel on the carbonyl carbon, the metabolic fate of the
larger fragment of lorlatinib resulting from this cleavage, the pyrido-pyrazole substructure,
could not be determined. In this current study, the radiolabel will be on the pyrazole ring
allowing for monitoring the metabolic fate of the pyrido-pyrazole part of the lorlatinib
molecule cleaved during the formation of the M8 metabolite. Since the M8 metabolite will not
be radiolabeled, its concentrations in plasma will be determined using a validated liquid
chromatography tandem mass spectrometric (LC/MS/MS) assay.
The sample size of approximately 6 was selected to ensure at least 4 fully evaluable subjects
with completed collections of plasma, urine, and fecal samples. This is a standard sample
size used for mass-balance/ADME studies which include assessment of metabolic profiling, and
is not based on empirical data or hypothesis testing criteria.
Metabolic profiling of radiolabeled components will be performed on pooled plasma samples as
well as on cumulative urine and feces excreted until Day 14 postdose or until one of the
early release criteria is met. The early release criteria are: 1) recovery in excreta of at
least 90% of administered radioactivity, or 2) less than 1% of administered radioactivity
being recovered in excreta from two consecutive days (ie, total for urine + feces should be
<1% on 2 consecutive days). Plasma concentrations of both lorlatinib and its unlabeled M8
metabolite will be analyzed using validated assays. Information from this study will
complement the metabolic profiling results from study B7461004, will help guide in the
assessment of potential drug-drug interactions (DDIs) and the need for other DDI studies with
lorlatinib, and will aid in the understanding of the possible causes for the unexpected
findings from a DDI study where a single 100 mg dose of lorlatinib was co-administered with
600 mg rifampin QD (study B7461011).
Banked biospecimens will be collected for the purpose of conducting research; specific uses
are described in the Banked Biospecimens section. Comparing the deoxyribonucleic acid (DNA),
ribonucleic acid (RNA), protein, and metabolite variation patterns of subjects who respond
well and those who respond poorly to treatment may help to better define the most appropriate
group of subjects in which to target a given treatment. Collecting biospecimens for
exploratory pharmacogenomic/genomic/biomarker analyses and retaining them in the Biospecimen
Banking System (BBS) make it possible to better understand the investigational product's
mechanism of action and to seek explanations for differences in, for example, exposure,
tolerability, safety, and/or efficacy not anticipated prior to the beginning of the study.
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