Anemia Clinical Trial
Official title:
Aging of Hematopoietic Stem Cells - Molecular Architecture of Marrow Dysplasia and Clinical Contribution of Ineffective Hematopoiesis to Frailty in the Elderly
The prevalence and incidence of anemia tend to increase with advancing age. Relatively low
hemoglobin concentrations are a common laboratory finding in the elderly, for the most part
judged by physicians as a sign without clinical relevance or as a marker of an underlying
chronic disease having no independent influence on health.
In recent years several studies have started to challenge the widespread and
self-perpetuating perception of anemia as an innocent bystander, reporting worse cognitive
and quality of life outcomes and increased risk of hospitalization and mortality in the
general population. Focusing on elderly people, anemia has a clear association with the
phenotypic features of frailty syndrome affecting 3-5% of individuals of 65-70 years of age
and, more importantly 30% of those aged 85 years or older.
Among frail older adults, anemia is a powerful prognostic factor for the development of
frailty-related problems such as muscle weakness, reduced performance, falls, and mortality.
Nutrient deficiency, chronic inflammation and renal insufficiency account for the large
majority of cases of anemia in the elderly, while underlying cause remained unexplained in
25% of the cases. Preliminary evidence indicates that a significant proportion of
''unexplained anemia'' may account for myelodysplasia(MDS). MDS is a condition typically
occurring in elderly people, characterized by clonal proliferation of hematopoietic stem
cells (HSC), which partly retain their capacity to differentiate and maturate, but do so in
an inefficient manner (ineffective hematopoiesis). Anemia represents the most important
prognostic factor in MDS. With time a portion of patients evolve into overt myeloid
malignancy (i.e., acute leukemia).
Somatic mutations occur in the genomes of healthy HSC at a low, but detectable frequency
during normal DNA replication. Although most mutations are rapidly corrected by DNA repair
mechanisms, those that persist are propagated during HSC self-renewal. Some evidence suggest
that these early driver mutations dictate future trajectories of evolution with distinct
clinical phenotypes. There has been much excitement in the research community about the
translational opportunities offered by genome sequencing, possibly leading to the
identification of specific types of mutational processes of how genome interact with
environmental factors in determining clinical conditions associated with aging and to the
implementation of a personalized molecular diagnosis and treatment for every patient. In this
translational research project, using an integrated genomic analysis based on next generation
sequencing (NGS) technologies,the investigators plan to dissect the genomic architecture of
MDS, significantly contributing to many features of frailty and to individual vulnerability.
The investigators will perform mutation analysis of candidate genes in a large and well
characterized cohort of individuals belonging to the "Health and Anemia'' study. "Health and
Anemia" is a prospective population-based observational study (2003-2013) of all elderly
residents in the municipality of Biella, Piedmont, a town in the north-west of Italy.
Hematological parameters together with data on cognition and functional status, mood and
quality of life, fatigue, hospitalization and mortality were collected for all patients.
Moreover, complete information on the development of hematological malignancies was provided
by local tumor registry up to 2018. The investigators aim to identify genes associated with
the induction of clonal hematopoiesis in elderly people, and then to correlate somatic
mutations with clinical/hematological features and progression into MDS and/or overt
leukemia. Moreover, The investigators will genotype single-cell-derived hematopoietic
colonies from CD34+ compartments (hematopoietic stem cells, multipotent progenitors, common
myeloid progenitors, and granulocyte progenitors) in order to clarify the clonal architecture
of marrow dysplasia in HSC, the dynamics of clonal establishment and expansion during
hematopoietic differentiation, and their relationship with the disease phenotype and
evolution. Finally, by analysing clinical data from "Health and Anemia study" the
investigators will investigate the clinical contribution of myelodysplasia-related anemia to
the development of frailty syndrome and its clinical sequela. The definition of molecular
architecture of marrow dysplasia would allow us to improve the current diagnosis and
classification of anemia in the elderly and the assessment of individual patient's risk of
disease associated morbidity/mortality. Finally, in patients with marrow dysplasia, gene
sequencing is expected to predict the vulnerability of a particular genotype to specific
treatment, thus providing a basis for optimizing at individual level timing and modality of
therapeutic intervention. The study population of the MOnzino 80-plus study will be used as
validation cohort.
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