Role of prolactin in lymphoid tissues of well-nourished and energy-restricted postpartum rats

馮堅持, Feng, Jianchi.

January 1998

published_or_final_version / Physiology / Doctoral / Doctor of Philosophy

Prolactin.

Lymphoid tissues.

Rats.

Role of prolactin in lymphoid tissues of well-nourished and energy-restricted postpartum rats /

Feng, Jianchi.

January 1998

Thesis (Ph. D.)--University of Hong Kong, 1999. / Includes bibliographical references (leaves 197-225).

Prolactin. Lymphoid tissues. Rats.

Compartmentalization of HIV-1 in the Secondary Lymphoid Tissues

Gregson, James Peter

02 August 2007

Follicular dendritic cells (FDCs) reside in the lymphoid follicles of the secondary lymphoid tissues (sLTs). Following the infection of an individual with human immunodeficiency virus type 1 (HIV-1), viral particles are trapped in massive quantities on the surfaces of FDCs. HIV-1 viral compartments are cell types or tissues between which there is a restriction of virus flow. Compartmentalization of HIV-1 creates numerous sites within the body in which the virus can undergo independent evolution, giving rise to a more diverse total viral population. Given the sessile nature of the FDC, I hypothesized that contrary to common assumptions, FDC-trapped HIV-1 is compartmentalized between different sLTs. Furthermore, given that FDC-trapped HIV-1 represents the major source of virus in the host, I postulated that this compartmentalization would likely impact the diversity of HIV-1 associated with the sLTs. I isolated FDCs, macrophages, and T cells from various sLTs, and sequenced cloned HIV-1 associated with these three cell populations. I subjected the resulting DNA and cDNA sequence data to phylogenetic and other statistical analyses. In support of my hypothesis, I demonstrate that both HIV-1 gp120 and pol sequences cloned from FDCs are compartmentalized between different sLTs. This compartmentalization is even apparent between lymph nodes taken from the same lymph node chain. One of the apparent effects of this compartmentalization is to significantly increase the viral genetic diversity in multiple sLTs when compared with diversity in a single sLT. It also appears that the selective pressures on HIV-1 differ among the sLTs. In addition, when proviruses isolated from macrophages from different sLTs were compared, it was also evident that there is compartmentalization of HIV-1 associated with this cell type as well. Finally, I demonstrate that HIV-1 isolated from an unfractionated population of cells from a single sLT, may be an inadequate representation of the total viral population in that sLT. Taken together, my data suggest that the nature of HIV-1 in the sLTs may be more complex than currently appreciated.

follicular dendritic cells

secondary lymphoid tissues

human immunodeficiency virus type 1

compartmentalization

Biochemistry

Chemistry

Dendritic Cells Enhance HIV Infection of Memory CD4+ T Cells in Human Lymphoid Tissues

Reyes-Rodriguez, Angel L.

27 January 2016

No description available.

Molecular Biology

Immunology

Cellular Biology

Virology

Lymphocytes T et vieillissement : lymphopénie ou redistribution ? / Lymphocytes T and Ageing : Lymphopenia or Redistribution ?

Martinet, Kim

23 September 2014

L’atteinte de l’âge sur les populations lymphocytaires T conventionnelles CD4 et CD8 avec l’avancée en âge est relativement bien décrite en périphérie lymphoïde secondaire chez la souris, et dans le sang périphérique chez l’homme. Deux paramètres sont observés : réduction du nombre de ces cellules et altération du ratio naïve/mémoire. À l’inverse, l’évaluation des tissus lymphoïdes tertiaires et des tissus extra lymphoïdes dans les réponses immunes, reste à affiner. Notre étude au cours du vieillissement physiologique du compartiment T fut menée dans des tissus lymphoïdes et non lymphoïdes de souris C57BL/6 wild-type, âgées entre 2 et 6 mois, entre 10 et 14 mois et entre 22 et 26 mois. Nous avons démontré que la lymphopénie T classiquement décrite liée au vieillissement dans les organes lymphoïdes secondaires ne s’applique pas à tout l’organisme : les compartiments intestinaux étudiés présentent une accumulation de cellules TCRαβ+ CD4+ (TCD4) et CD8+ (TCD8). Nos résultats dévoilent un impact différentiel du vieillissement sur le nombre absolu des différents compartiments cellulaires TCRαβ+ dans les organes lymphoïdes et la muqueuse intestinale. Ces résultats suggèrent donc que la lymphopénie T décrite dans les organes lymphoïdes s’établissant au cours du vieillissement pourrait être essentiellement liée à une redistribution des lymphocytes. A l’inverse, la persistance des cellules T régulatrices dans les organes lymphoïdes secondaires pourrait être liée à une production locale dans la muqueuse intestinale. Il semble donc que l’équilibre TCD8/TCD4 peut être différemment affecté selon le site considéré et cette observation peut fournir une justification pour la plus grande susceptibilité aux infections observée avec l’âge. / Consequences of ageing on conventional CD4 and CD8 T lymphocytes populations is relatively well described in murine secondary lymphoid organs and in human peripheral blood: reduction the number of these cells and alteration of naïve/effector-memory ratio in favour of effector-memory cells. Conversely, evaluation in tertiary lymphoid tissues and non-lymphoid tissues remains to be refined. We conducted an exhaustive analysis of T cell compartments during physiological aging in lymphoid and non-lymphoid tissues isolated from wild-type C57BL/6 mice aged of 2 to 6 months, 10 to 14 months and 22 to 26 months. We demonstrated that T lymphopenia described classically associated with aging in the secondary lymphoid organs does not apply to the whole organism: intestinal compartments studied show an accumulation of TCRαβ+ CD4+ cells (TCD4) and CD8+ (TCD8). Our results reveal a differential impact of aging on the absolute number of different TCRαβ+ cellular compartments in lymphoid organs and intestinal mucosa. T cell lymphopenia in secondary lymphoid organs currently associated to ageing may essentially reflect T cell redistribution. TCD8/TCD4 balance may be affected differently depending on the site considered and this observation may provide a rationale for the greater susceptibility to infection observed with age.

Age

Vieillissement

Immunosénescence

Homéostasie des lymphocytes T

Lymphopénie

Lymphocytopénie T

MALT, mucosa associated lymphoid tissues

GALT, gut associated lymphoid tissues

Lamina propria

Hétérogénéité anatomique

Age

Ageing

Immunosenescence

T cell homeostasis

Lymphopenia

T lymphopenia

MALT, mucosa associated lymphoid tissue

GALT, gut associated lymphoid tissue

Lamina propria

Anatomical heterogeneity

Établissement et persistance du réservoir du VIH chez des individus traités très tôt en phase aigüe de l’infection (cohorte RV254)

Leyre, Louise

08 1900

No description available.

Réservoir du VIH

Infection aigüe

Traitement précoce

Tissus lymphoïdes

Cellules T CD4+ mémoires

HIV reservoir

Acute infection

Early treatment

Lymphoid tissues

Memory CD4+ T cells