Lipoprotein Lipase Deficiency Clinical Trial
Official title:
A Clinical Records Review Study of the Frequency and Severity of Acute Abdominal "Pancreatitis" Episodes Reported From LPLD Subjects Previously Recruited to Clinical Studies PREPARATION-02, CT-AMT-011-01 and CT-AMT-011-02
Lipoprotein lipase deficiency (LPLD) is an autosomal recessive inherited condition caused by
homozygosity or compound heterozygosity for mutations within the LPL gene. LPLD results in
subjects presenting with fasting plasma triglyceride (TG) levels of > 10 mmol/l. LPLD
typically presents in infancy or childhood with usual complaints of severe abdominal pain,
repetitive colicky pains and repeated episodes of acute pancreatitis The most severe
clinical complication associated with LPLD is acute pancreatitis. Pancreatitis in an LPLD
subject often leads to prolonged hospital admissions (sometimes up to weeks). Subjects who
survive repeated episodes of acute pancreatitis may develop chronic pancreatitis, ultimately
resulting in endocrine and exocrine pancreatic insufficiency.
The clinical manifestations of acute pancreatitis episodes related to LPLD are largely
indistinguishable from acute pancreatitis due to other causes. However, collection of data
relating to hospital admissions, laboratory test results, scan images and adverse events
occurring concomitantly to the acute pancreatic episode should allow elimination of other
causes of pancreatitis (e.g gallstones etc) and ultimately allow confirmation of
LPLD-related acute pancreatitis. Characterization of the presentation of symptoms which
occur around the time of known episodes of LPLD-related acute pancreatitis should also
permit identification of episodes of acute pancreatitis which have previously been
considered as unrelated or even unrecognized.
The objective of the study is to re-assess and re-confirm data previously recorded about the
incidence and severity of acute abdominal "pancreatitis" episodes in LPLD subjects
previously enrolled on AMT clinical studies. To assess and document the presentation of
acute abdominal episodes that occur around known episodes of pancreatitis and to permit the
identification of possible new previously unrecorded episodes of pancreatitis based upon
predefined diagnostic criteria. The objective is to recruit the 27 subjects previously
enrolled in the above mentioned clinical studies.
Lipoprotein lipase deficiency (LPLD) is an autosomal recessive inherited condition caused by
homozygosity or compound heterozygosity for mutations within the LPL gene.
The most severe clinical complication associated with LPLD is acute pancreatitis.
Pancreatitis in an LPLD subject often leads to prolonged hospital admissions. Subjects who
survive repeated episodes of acute pancreatitis may develop chronic pancreatitis, ultimately
resulting in endocrine and exocrine pancreatic insufficiency.
The clinical manifestations of acute pancreatitis episodes related to LPLD are largely
indistinguishable from acute pancreatitis due to other causes. However, collection of data
relating to hospital admissions, laboratory test results, scan images and adverse events
occurring concomitantly to the acute pancreatic episode should allow elimination of other
causes of pancreatitis (e.g. gallstones etc) and ultimately allow confirmation of
LPLD-related acute pancreatitis. Characterisation of the presentation of symptoms which
occur around the time of known episodes of LPLD-related acute pancreatitis should also
permit identification of episodes of acute pancreatitis which have previously been
considered as unrelated or even unrecognized.
Alipogene tiparvovec (Glybera®) is in development for the therapy of LPLD. In summary,
alipogene tiparvovec contains the human lipoprotein (LPL) gene variant LPLS447X in a
non-replicating vector in solution administered in a one-time series of intramuscular
injections in the arms/legs.
Studies conducted to date with Glybera have evaluated total triglyceride levels as a
surrogate marker for efficacy and have not evaluated a clinical endpoint such as acute
pancreatitis episodes as a primary endpoint. Post-hoc analysis has suggested that there may
be a reduction in the frequency of acute abdominal pancreatitis episodes reported following
treatment compared to the frequency reported pre-treatment from past medical history
records. The recorded episodes used in this post-hoc analysis were collected from medical
history and adverse event data but no uniform criteria were used to classify these as
episodes of acute pancreatitis. Review of the post hoc analysis has raised questions that
the recorded past medical history of pancreatitis episodes may be inaccurate with respect to
diagnosis and number of episodes.
In this case record review study, data will be collected on pancreatitis episodes from
subjects who previously enrolled in studies PREPARATION-02 (observational), CT-AMT-011-01
and CT-AMT-011-02. In studies CT-AMT-011-01 and CT-AMT-011-02 subjects received AMT-011 at
either dose 3 x 1011 gc/kg or 1 x 1012 gc/kg. Data obtained from medical records, hospital
admission/discharge charts, laboratory results and imaging scans will be evaluated for
evidence of LPLD-related episodes of pancreatitis by an expert review panel. The evaluation
will consider data collected from three time periods:
- subjects entire past medical history,
- the period after enrolment into study but prior to AMT-011 therapy,
- the period post-administration of AMT-011.
Data from the subjects who did not progress to receive AMT-011 will be evaluated as a
control group using data collected from past medical history and from the period after
enrolment in the PREPARATION-02.
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