Liver Cancer Clinical Trial
Official title:
A Worldwide Usable Scoring System for Patients With Hepatocellular Cancer Waiting for Liver Transplantation
The present study has been developed with multiple aims: 1) to refine available models for liver transplantation which would be able to cover the fate of HCC candidates from an ITT point of view; 2) to develop such an approach on cohorts coming from both Eastern and Western countries; 3) to maintain simplicity of use; 4) to provide individual prognostication taking into account different causes of death, through a competing-risk model; 5) to provide an external validation on cohorts coming from both Eastern and Western countries. All these aims converge at providing a comprehensive and useful assessment suitable for both candidates selection and allocation priority.
For two decades, the Milan Criteria (MC) have represented the cornerstone in the selection of
patients with hepatocellular cancer (HCC) as candidates for liver transplantation (LT). Since
then, several Western and Eastern centres have tried to overcome MC stringency with the aim
to expand the number of potentially transplantable patients without increasing the risk of
post-LT tumour recurrence. Recently, variables correlated with HCC biology have been
introduced to capture its aggressiveness and suitability for LT. Among the most commonly
proposed, we can cite the alpha-fetoprotein (AFP) and the radiological response after
neo-adjuvant loco-regional treatments (LRT). The effort to combine HCC morphology and biology
is now emerging as the more promising approach for further refining the selection process of
HCC candidates. The recently proposed prognostic indexes Metroticket 2.0,
Time-Radiological-response-Alpha-fetoprotein-INflammation (TRAIN), Model Of Recurrence After
Liver transplant (MORAL) and French AFP-model represent the most promising results of such
planned endeavours.
With the intent to be clinically useful, a prognostic system must achieve not only the most
common performance metrics, such as discrimination and calibration, but also an adequate
coverage of the population in which it would be applied. It can be argued that a prognostic
system based only on criteria available at the moment of LT could not satisfy such a
pre-requisite when the entire population of HCC patients waiting in the list for LT is taken
into account, considering an intention-to-treat (ITT) point of view. In this sense, only the
TRAIN system developed an ITT analysis, whereas the remaining were all based on
pre-transplant information. The second quality that a clinically useful prognostic system
should have is its immediacy. Thus, it should be based on commonly available information, not
requiring additional analyses or exams if not justified by a substantial improvement in
accuracy. Last but not least, a prognostic system should also provide for an individual
prediction in addition to risk-stratification, with the intent to offer personalized
prognostication for each different patient. To date, only the Metroticket 2.0 fulfils these
two last requisites. A final important quality of the Metroticket 2.0 is that it applied a
competing-risk analysis able to clean up the HCC-related cause of death from other
non-tumour-related causes.
On this background, we developed the present study with multiple aims: 1) to refine available
models which would be able to cover the fate of HCC candidates from an ITT point of view; 2)
to develop such an approach on cohorts coming from both Eastern and Western countries; 3) to
maintain simplicity of use; 4) to provide individual prognostication taking into account
different causes of death, through a competing-risk model; 5) to provide an external
validation on cohorts coming from both Eastern and Western countries. All these aims converge
at providing a comprehensive and useful assessment suitable for both candidates selection and
allocation priority.
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