Author: Takamura, Shiki
Title: Persistence in Temporary Lung Niches: A Survival Strategy of Lung-Resident Memory CD8(+) T Cells Document date: 2017_7_1
ID: 2klytw6c_8
Snippet: New definitions provided by intravascular staining Intravascular (i.v.) staining of cells in the bloodstream by i.v. injection with specific antibodies before harvesting the cells has revolutionized the analysis of lung T RM (5, 6) . Since the lung is a highly vascularized organ, it became apparent that a majority of CD8 + T cells purified from the lung tissues in earlier studies were contaminants from the blood. In fact, >95% of total CD8 + T ce.....
Document: New definitions provided by intravascular staining Intravascular (i.v.) staining of cells in the bloodstream by i.v. injection with specific antibodies before harvesting the cells has revolutionized the analysis of lung T RM (5, 6) . Since the lung is a highly vascularized organ, it became apparent that a majority of CD8 + T cells purified from the lung tissues in earlier studies were contaminants from the blood. In fact, >95% of total CD8 + T cells in naive animals and *50% of antigen-specific memory CD8 + T cells in mice that had recovered from an influenza virus infection were found to be derived from the lung vasculature (6, 126) . Note that because the lung airways are segregated from the blood vessels, i.v. staining has essentially no impact on the cells in these tissues. However, a careful reinterpretation of previously published data regarding cells in the lung interstitium/parenchyma analyzed without i.v. staining is required. For instance, it has been reported that antigen-specific CD8 + T cells generated by intraperitoneal infections were efficiently recruited to the interstitium/parenchyma, but not to the lung airways when the effector T cell numbers peak (9-11 days) even in the absence of progressive infection or inflammation in the lung (122) . Furthermore, parabiosis experiments in which pairs of mice are surgically joined revealed that significant numbers of memory CD8 + T cells could also be recruited to the lung as up to half of the cells in this organ were replaced by circulatory CD8 + T cell populations (63, 84) . By using i.v. staining, those conclusions have been revised. First, although effector CD8 + T cells migrate into the interstitium of normal lungs more efficiently than naive CD8 + T cells (33) , the extent is much less than that observed in the presence of infection/inflammation in the lung (123) . Second, the migration of circulating memory CD8 + T cells to the lung under steady-state conditions is also relatively limited, as the ratio of new immigrants to resident cells never exceeds 20% (123) . On the basis of these new findings, we propose that the migration of effector as well as naive /memory CD8 + T cells into the noninflamed lung be termed as ''basal recruitment'' and be distinguished from ''active recruitment'': migration of antigen-specific effector CD8 + T cells to the lung in response to inflammation in the tissues (Fig. 1) . Strict discrimination between basal and active recruitment is important because tissue-derived instructive factors (e.g., antigen and inflammatory stimuli) that dictate T RM differentiation differs significantly depending on how the cells were recruited.
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