TY - JOUR
T1 - Increased proliferation of B cells and auto-immunity in mice lacking protein kinase Cδ
AU - Miyamoto, Akitomo
AU - Nakayama, Keiko
AU - Imaki, Hiroyuki
AU - Hirose, Sachiko
AU - Jiang, Yi
AU - Abe, Masaaki
AU - Tsukiyama, Tadasuke
AU - Nagahama, Hiroyasu
AU - Ohno, Shigeo
AU - Hatakeyama, Shigetsugu
AU - Nakayama, Keiichi I.
N1 - Funding Information:
We thank C. Goodnow, J. Cyster and F. Finkelman for providing reagents; members of the Laboratory for Lymphocyte Signaling in Cologne for technical assistance; and G. Hannon for the preparation of the manuscript. We thank M. Nussenzweig, D. O0Carrol, K. Rajewsky and C. Schmedt for discussion. This work was supported by The Irene Diamond Fund (A.T.) and National Institutes of Health grant (N-Y.Z. and A.T.), S. L. E. Foundation (K.S.), Graduiertenkolleg from the Deutsche Forschungsgemeinschaft, and The Rockefeller University’s Women & Science Fellowship Program (I.M.).
Funding Information:
We thank S. Akira and K. Hoshino for the plasmids; N. Motoyama, A. Yoshimura and U. Kikkawa for discussions; Y. Yamada, K. Shimoharada and N. Ohtsuji for technical assistance; and M. Kimura and C. Sugita for help in preparation of the manuscript. This work was supported in part by a grant from the Ministry of Education, Science, Sports and Culture of Japan, by Nissan Science Foundation, and by a research grant from the Human Frontier Science Program.
PY - 2002/4/25
Y1 - 2002/4/25
N2 - Protein kinase C (PKC), which comprises 11 closely related isoforms, has been implicated in a wide variety of cellular processes, such as growth, differentiation, secretion, apoptosis and tumour development1-4. Among the PKC isotypes, PKC-δ is unique in that its overexpression results in inhibition of cell growth5-11. Here we show that mice that lack PKC-δ exhibit expansion of the B-lymphocyte population with the formation of numerous germinal centres in the absence of stimulation. The rate of proliferation in response to stimulation was greater for B cells from PKC-δ-deficient mice than for those from wild-type mice. Adoptive transfer experiments suggested that the hyperproliferation phenotype is B-cell autonomous. Production of interleukin-6 was markedly increased in B cells of PKC-δ-null mice as a result of an increase in the DNA-binding activity of NF-IL6. Furthermore, the PKC-δ-deficient mice contain circulating autoreactive antibodies and display immune-complex-type glomerulonephritis, as well as lymphocyte infiltration in many organs. These results suggest that PKC-δ has an indispensable function in negative regulation of B-cell proliferation, and is particularly important for the establishment of B-cell tolerance.
AB - Protein kinase C (PKC), which comprises 11 closely related isoforms, has been implicated in a wide variety of cellular processes, such as growth, differentiation, secretion, apoptosis and tumour development1-4. Among the PKC isotypes, PKC-δ is unique in that its overexpression results in inhibition of cell growth5-11. Here we show that mice that lack PKC-δ exhibit expansion of the B-lymphocyte population with the formation of numerous germinal centres in the absence of stimulation. The rate of proliferation in response to stimulation was greater for B cells from PKC-δ-deficient mice than for those from wild-type mice. Adoptive transfer experiments suggested that the hyperproliferation phenotype is B-cell autonomous. Production of interleukin-6 was markedly increased in B cells of PKC-δ-null mice as a result of an increase in the DNA-binding activity of NF-IL6. Furthermore, the PKC-δ-deficient mice contain circulating autoreactive antibodies and display immune-complex-type glomerulonephritis, as well as lymphocyte infiltration in many organs. These results suggest that PKC-δ has an indispensable function in negative regulation of B-cell proliferation, and is particularly important for the establishment of B-cell tolerance.
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U2 - 10.1038/416865a
DO - 10.1038/416865a
M3 - Article
C2 - 11976687
AN - SCOPUS:0037171731
SN - 0028-0836
VL - 416
SP - 865
EP - 869
JO - Nature
JF - Nature
IS - 6883
ER -