AI Article Synopsis

  • The study investigates how T lymphocytes contribute to maternal-to-neonatal immunity during breastfeeding, specifically examining their presence in the mammary gland under normal and infection-stimulated conditions.
  • It was found that T cell numbers peak during late pregnancy but significantly decline during early lactation, suggesting that some T cells may be transferred into the milk for the neonate's immunity.
  • In cases of maternal infection (specifically with Trichinella spiralis), a notable decrease in T cells was observed in the mammary tissue during early lactation, hinting at a greater loss of T cells to milk compared to non-infected controls.

Article Abstract

We have shown that antigen-specific T lymphocytes can mediate maternal-to-neonatal immunity during lactation. Present studies address the dynamics of lymphocyte accumulation in the mammary gland during normal and disease stimulated conditions. Monoclonal antibodies specific for total T cells, suppressor/cytotoxic and helper subsets, and macrophages were used in conjunction with immunohistochemistry to identify and count the individual cell types. In unstimulated mammary tissue, following a rise in T cells to maximal numbers in late pregnancy, the total number of T cells/high power field (HPF) was significantly diminished in early lactation and continued to decline to the late lactation period. Both the numbers of T cells/HPF located in the mammary alveolar epithelium and surrounding connective tissue were significantly reduced in early lactation as compared to late pregnancy. This indicates the possible passage of cells into the milk during lactation. Prior infection of the mother with Trichinella spiralis and a secondary challenge 48 h. before sacrifice caused a significant reduction in the number of T cells in the mammary tissue in early lactation as compared with unstimulated controls, indicating the possibility of an even greater outflow of T cells into milk. In controls, the T-suppressor/cytotoxic subtype showed a reduction in early lactation versus late pregnancy but showed no shifts in total cells/HPF during infection. The T-helper subtype in controls remained unchanged from late pregnancy to early lactation with a considerable decline in late lactation. However, the T-helper cells were significantly decreased in T. spiralis-treated animals as compared with noninfected controls in early lactation.(ABSTRACT TRUNCATED AT 250 WORDS)

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http://dx.doi.org/10.1002/ar.1092300212DOI Listing

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