PHENOTYPICAL CHARACTERIZATION OF CELLS IN THE THORACIC-DUCT OF PATIENTS WITH AND WITHOUT SYSTEMIC INFLAMMATORY RESPONSE SYNDROME AND MULTIPLE ORGAN FAILURE
Lcjm. Lemaire et al., PHENOTYPICAL CHARACTERIZATION OF CELLS IN THE THORACIC-DUCT OF PATIENTS WITH AND WITHOUT SYSTEMIC INFLAMMATORY RESPONSE SYNDROME AND MULTIPLE ORGAN FAILURE, Scandinavian journal of immunology, 47(1), 1998, pp. 69-75
The subset composition and recirculation properties of the migrating l
ymphocyte pool in humans is largely unknown. The present study was con
ducted in order to phenotypically characterize cells in human thoracic
duct lymph of patients under non-inflammatory and inflammatory condit
ions. These data were compared with data from peripheral blood, with s
pecial emphasis on those cells homing to the gut. Thoracic duct lymph
and peripheral blood contained comparable proportions of B and T lymph
ocytes and CD8(+) cells. Thoracic duct lymph contained proportionally
more CD4(+) cells, more CD4(+)CD45RO(+) that express alpha(4) beta(7)
cells and more CD8(+)CD45RO(+) that express alpha(4) beta(7), as compa
red to peripheral blood. These data suggest an equal recirculation rat
e of B and T lymphocytes; a more active recirculation of CD4(+) cells
compared to CD8(+) cells; and a more active recirculation of memory ce
lls to the gut as compared to other extra-lymphoid sites in patients u
nder non-inflammatory conditions. Data were also obtained in patients
with the system inflammatory response syndrome and multiple organ fail
ure. Although it is generally assumed that granulocytes and monocytes
do not recirculate, lymph of multiple organ failure patients contained
significantly more granulocytes than monocytes, indicating that in se
vere generalized inflammatory states these cells re-enter the circulat
ion through the thoracic duct. Furthermore, no increased activation of
cells homing to the gut was found in these patients.