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The role of the fibrocyte, a bone marrow-derived mesenchymal progenitor, in reactive and
MINI REVIEW
The role of the fibrocyte, a bone marrow-derived
mesenchymal progenitor, in reactive and
reparative fibroses
Alberto Bellini and Sabrina Mattoli
Human fibrocytes are mesenchymal progenitors that exhibit mixed morphological and molecular characteristics of
hematopoietic stem cells, monocytes and fibroblasts. They likely represent the obligate intermediate stage of differ-
entiation into mature mesenchymal cells of a bone marrow-derived precursor of the monocyte lineage under permissive
conditions. On in vitro stimulation with pro-fibrotic cytokines and growth factors, human fibrocytes produce large
quantities of extracellular matrix components and further differentiate into cells identical to the contractile myofibro-
blasts that emerge at the tissue sites during repair processes and in some fibrotic lesions. Studies in various animal
models of wound healing or fibrotic diseases have confirmed the ability of fibrocytes to differentiate into mature
mesenchymal cells in vivo and have suggested a causal link between fibrocyte accumulation and ongoing tissue fi-
brogenesis or vascular remodeling in response to tissue damage or hypoxia. Fibrocytes synthesizing new collagen or
acquiring myofibroblast markers have been detected in human hypertrophic scars, in the skin of patients affected by
nephrogenic systemic fibrosis, in human atherosclerotic lesions, and in pulmonary diseases characterized by repeated
cycles of inflammation and repair, like asthma. The presence of fibrocyte-like cells has been reported in human chronic
pancreatitis and chronic cystitis. Similar cells also populate the stroma surrounding human benign tumors. The available
data indicate that human fibrocytes serve as a source of mature mesenchymal cells during reparative processes and in
fibrotic disorders or stromal reactions predominantly associated with a persistent inflammatory infiltrate or with the
selective recruitment of monocytes induced by ischemic changes and tumor development. A d
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