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Reduced Cell Turnover in Bovine LeukemiaVirus-Infected, Persistently LymphocytoticCattle
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ABSTRACT
Although
nucleotide analogs like bromodeoxyuridine have been extensively used to
estimate cell proliferation in vivo, precise dynamic parameters are
scarce essentially because of the lack of adequate mathematical models.
Besides recent developments on T cell dynamics, the turnover rates of B
lymphocytes are largely unknown particularly in the context of a
virally induced pathological disorder. Here, we aim to resolve this
issue by determining the rates of cell proliferation and death during
the chronic stage of the bovine leukemia virus (BLV) infection, called
bovine persistent lymphocytosis (PL). Our methodology is based on
direct intravenous injection of bromodeoxyuridine in association with
subsequent flow cytometry. By this in vivo approach, we show that the
death rate of PL B lymphocytes is significantly reduced (average death
rate, 0.057 day
−1
versus 0.156
day
−1
in the asymptomatic controls). Concomitantly,
proliferation of the PL cells is also significantly restricted compared
to the controls (average proliferation rate, 0.0046
day
−1
versus 0.0085 day
−1
). We
conclude that bovine PL is characterized by a decreased cell turnover
resulting both from a reduction of cell death and an overall impairment
of proliferation. The cell dynamic parameters differ from those
measured in sheep, an experimental model for BLV infection. Finally,
cells expressing p24 major capsid protein ex vivo were not BrdU
positive, suggesting an immune selection against proliferating
virus-positive lymphocytes. Based on a comparative leukemia approach,
these observations might help to understand cell dynamics during other
lymphoproliferative disease such as chronic lymphocytic leukemia or
human T-cell lymphotropic virus-induced adult T-cell leukemia in
humans.
American Society for Microbiology
Title: Reduced Cell Turnover in Bovine LeukemiaVirus-Infected, Persistently LymphocytoticCattle
Description:
ABSTRACT
Although
nucleotide analogs like bromodeoxyuridine have been extensively used to
estimate cell proliferation in vivo, precise dynamic parameters are
scarce essentially because of the lack of adequate mathematical models.
Besides recent developments on T cell dynamics, the turnover rates of B
lymphocytes are largely unknown particularly in the context of a
virally induced pathological disorder.
Here, we aim to resolve this
issue by determining the rates of cell proliferation and death during
the chronic stage of the bovine leukemia virus (BLV) infection, called
bovine persistent lymphocytosis (PL).
Our methodology is based on
direct intravenous injection of bromodeoxyuridine in association with
subsequent flow cytometry.
By this in vivo approach, we show that the
death rate of PL B lymphocytes is significantly reduced (average death
rate, 0.
057 day
−1
versus 0.
156
day
−1
in the asymptomatic controls).
Concomitantly,
proliferation of the PL cells is also significantly restricted compared
to the controls (average proliferation rate, 0.
0046
day
−1
versus 0.
0085 day
−1
).
We
conclude that bovine PL is characterized by a decreased cell turnover
resulting both from a reduction of cell death and an overall impairment
of proliferation.
The cell dynamic parameters differ from those
measured in sheep, an experimental model for BLV infection.
Finally,
cells expressing p24 major capsid protein ex vivo were not BrdU
positive, suggesting an immune selection against proliferating
virus-positive lymphocytes.
Based on a comparative leukemia approach,
these observations might help to understand cell dynamics during other
lymphoproliferative disease such as chronic lymphocytic leukemia or
human T-cell lymphotropic virus-induced adult T-cell leukemia in
humans.
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