T helper cell trafficking in autoimmune kidney diseases

Jan-Hendrik Riedel; Jan-Eric Turner; Ulf Panzer

doi:10.1007/s00441-020-03403-6

T helper cell trafficking in autoimmune kidney diseases

Standard

T helper cell trafficking in autoimmune kidney diseases. / Riedel, Jan-Hendrik ; Turner, Jan-Eric ; Panzer, Ulf.

In: CELL TISSUE RES, Vol. 385, No. 2, 08.2021, p. 281-292.

Research output: SCORING: Contribution to journal › SCORING: Review article › Research

Harvard

Riedel, J-H , Turner, J-E & Panzer, U 2021, 'T helper cell trafficking in autoimmune kidney diseases', CELL TISSUE RES, vol. 385, no. 2, pp. 281-292. https://doi.org/10.1007/s00441-020-03403-6

APA

Riedel, J-H., Turner, J-E., & Panzer, U. (2021). T helper cell trafficking in autoimmune kidney diseases. CELL TISSUE RES, 385(2), 281-292. https://doi.org/10.1007/s00441-020-03403-6

Vancouver

Riedel J-H , Turner J-E , Panzer U. T helper cell trafficking in autoimmune kidney diseases. CELL TISSUE RES. 2021 Aug;385(2):281-292. https://doi.org/10.1007/s00441-020-03403-6

Bibtex

@article{a59a0be79dac469aa2735d3624c251d6,

title = "T helper cell trafficking in autoimmune kidney diseases",

abstract = "CD4+ T cells are key drivers of autoimmune diseases, including crescentic GN. Many effector mechanisms employed by T cells to mediate renal damage and repair, such as local cytokine production, depend on their presence at the site of inflammation. Therefore, the mechanisms regulating the renal CD4+ T cell infiltrate are of central importance. From a conceptual point of view, there are four distinct factors that can regulate the abundance of T cells in the kidney: (1) T cell infiltration, (2) T cell proliferation, (3) T cell death and (4) T cell retention/egress. While a substantial amount of data on the recruitment of T cells to the kidneys in crescentic GN have accumulated over the last decade, the roles of T cell proliferation and death in the kidney in crescentic GN is less well characterized. However, the findings from the data available so far do not indicate a major role of these processes. More importantly, the molecular mechanisms underlying both egress and retention of T cells from/in peripheral tissues, such as the kidney, are unknown. Here, we review the current knowledge of mechanisms and functions of T cell migration in renal autoimmune diseases with a special focus on chemokines and their receptors.",

author = "Jan-Hendrik Riedel and Jan-Eric Turner and Ulf Panzer",

year = "2021",

month = aug,

doi = "10.1007/s00441-020-03403-6",

language = "English",

volume = "385",

pages = "281--292",

journal = "CELL TISSUE RES",

issn = "0302-766X",

publisher = "Springer",

number = "2",

}

RIS

TY - JOUR

T1 - T helper cell trafficking in autoimmune kidney diseases

AU - Riedel, Jan-Hendrik

AU - Turner, Jan-Eric

AU - Panzer, Ulf

PY - 2021/8

Y1 - 2021/8

N2 - CD4+ T cells are key drivers of autoimmune diseases, including crescentic GN. Many effector mechanisms employed by T cells to mediate renal damage and repair, such as local cytokine production, depend on their presence at the site of inflammation. Therefore, the mechanisms regulating the renal CD4+ T cell infiltrate are of central importance. From a conceptual point of view, there are four distinct factors that can regulate the abundance of T cells in the kidney: (1) T cell infiltration, (2) T cell proliferation, (3) T cell death and (4) T cell retention/egress. While a substantial amount of data on the recruitment of T cells to the kidneys in crescentic GN have accumulated over the last decade, the roles of T cell proliferation and death in the kidney in crescentic GN is less well characterized. However, the findings from the data available so far do not indicate a major role of these processes. More importantly, the molecular mechanisms underlying both egress and retention of T cells from/in peripheral tissues, such as the kidney, are unknown. Here, we review the current knowledge of mechanisms and functions of T cell migration in renal autoimmune diseases with a special focus on chemokines and their receptors.

AB - CD4+ T cells are key drivers of autoimmune diseases, including crescentic GN. Many effector mechanisms employed by T cells to mediate renal damage and repair, such as local cytokine production, depend on their presence at the site of inflammation. Therefore, the mechanisms regulating the renal CD4+ T cell infiltrate are of central importance. From a conceptual point of view, there are four distinct factors that can regulate the abundance of T cells in the kidney: (1) T cell infiltration, (2) T cell proliferation, (3) T cell death and (4) T cell retention/egress. While a substantial amount of data on the recruitment of T cells to the kidneys in crescentic GN have accumulated over the last decade, the roles of T cell proliferation and death in the kidney in crescentic GN is less well characterized. However, the findings from the data available so far do not indicate a major role of these processes. More importantly, the molecular mechanisms underlying both egress and retention of T cells from/in peripheral tissues, such as the kidney, are unknown. Here, we review the current knowledge of mechanisms and functions of T cell migration in renal autoimmune diseases with a special focus on chemokines and their receptors.

U2 - 10.1007/s00441-020-03403-6

DO - 10.1007/s00441-020-03403-6

M3 - SCORING: Review article

C2 - 33598825

VL - 385

SP - 281

EP - 292

JO - CELL TISSUE RES

JF - CELL TISSUE RES

SN - 0302-766X

IS - 2

ER -