PKCδ is dispensible for oxLDL uptake and foam cell formation by human and murine macrophages

Katka Szilagyi; Alexander B. Meijer; Annette E. Neele; Paul Verkuijlen; Michael Leitges; Sandrine Dabernat; Elisabeth Förster-Waldl; Kaan Boztug; Alexandre Belot; Taco W. Kuijpers; Georg Kraal; Menno P. J. de Winther; Timo K. van den Berg; E. Forster-Waldl

doi:10.1093/cvr/cvu213

PKCδ is dispensible for oxLDL uptake and foam cell formation by human and murine macrophages

Katka Szilagyi
, Alexander B. Meijer
, Annette E. Neele
, Paul Verkuijlen
, Michael Leitges
, Sandrine Dabernat
, Elisabeth Förster-Waldl
, Kaan Boztug
, Alexandre Belot
, Taco W. Kuijpers
, Georg Kraal
, Menno P. J. de Winther
, Timo K. van den Berg
, E. Forster-Waldl

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Uptake of oxidized lipoprotein particles (oxLDL) and foam cell formation by macrophages is one of the first steps in the development of atherosclerosis. Recently, protein kinase C δ (PKCδ) has been implicated as a regulator of oxLDL uptake and foam cell formation via down-regulation of PKCβ and scavenger receptors CD36 and SR-A expression. Here, we describe studies in which we have re-evaluated the role of PKCδ in oxLDL uptake and foam cell formation. PKCδ expression was silenced in the human monocytic cell lines and also in primary human monocytes to analyse oxLDL uptake and CD36 expression. Additionally, bone marrow-derived macrophages of PKCδ knockout mice and macrophages cultured from patients with rare null mutations in the PRKCD gene were tested for uptake of oxLDL and foam cell formation. Expression of scavenger receptor CD36 was determined and levels of PKCβ isoforms were quantified. Neither a reduction in PKCδ levels nor its complete absence resulted in a detectable effect on the uptake of oxLDL and the formation of foam cells. PKCδ is dispensible for oxLDL uptake and foam cell formation by monocytes and macrophages

Original language	English
Pages (from-to)	467-476
Journal	Cardiovascular research
Volume	104
Issue number	3
DOIs	https://doi.org/10.1093/cvr/cvu213
Publication status	Published - 2014

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SDG 3 Good Health and Well-being

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10.1093/cvr/cvu213

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Szilagyi, K., Meijer, A. B., Neele, A. E., Verkuijlen, P., Leitges, M., Dabernat, S., Förster-Waldl, E., Boztug, K., Belot, A., Kuijpers, T. W., Kraal, G., de Winther, M. P. J., van den Berg, T. K., & Forster-Waldl, E. (2014). PKCδ is dispensible for oxLDL uptake and foam cell formation by human and murine macrophages. Cardiovascular research, 104(3), 467-476. https://doi.org/10.1093/cvr/cvu213

@article{dd0455c660e4444daa251f11998eb2b5,

title = "PKCδ is dispensible for oxLDL uptake and foam cell formation by human and murine macrophages",

abstract = "Uptake of oxidized lipoprotein particles (oxLDL) and foam cell formation by macrophages is one of the first steps in the development of atherosclerosis. Recently, protein kinase C δ (PKCδ) has been implicated as a regulator of oxLDL uptake and foam cell formation via down-regulation of PKCβ and scavenger receptors CD36 and SR-A expression. Here, we describe studies in which we have re-evaluated the role of PKCδ in oxLDL uptake and foam cell formation. PKCδ expression was silenced in the human monocytic cell lines and also in primary human monocytes to analyse oxLDL uptake and CD36 expression. Additionally, bone marrow-derived macrophages of PKCδ knockout mice and macrophages cultured from patients with rare null mutations in the PRKCD gene were tested for uptake of oxLDL and foam cell formation. Expression of scavenger receptor CD36 was determined and levels of PKCβ isoforms were quantified. Neither a reduction in PKCδ levels nor its complete absence resulted in a detectable effect on the uptake of oxLDL and the formation of foam cells. PKCδ is dispensible for oxLDL uptake and foam cell formation by monocytes and macrophages",

author = "Katka Szilagyi and Meijer, \{Alexander B.\} and Neele, \{Annette E.\} and Paul Verkuijlen and Michael Leitges and Sandrine Dabernat and Elisabeth F{\"o}rster-Waldl and Kaan Boztug and Alexandre Belot and Kuijpers, \{Taco W.\} and Georg Kraal and \{de Winther\}, \{Menno P. J.\} and \{van den Berg\}, \{Timo K.\} and E. Forster-Waldl",

year = "2014",

doi = "10.1093/cvr/cvu213",

language = "English",

volume = "104",

pages = "467--476",

journal = "Cardiovascular research",

issn = "0008-6363",

publisher = "Oxford University Press",

number = "3",

}

Szilagyi, K, Meijer, AB, Neele, AE, Verkuijlen, P, Leitges, M, Dabernat, S, Förster-Waldl, E, Boztug, K, Belot, A, Kuijpers, TW, Kraal, G, de Winther, MPJ , van den Berg, TK & Forster-Waldl, E 2014, 'PKCδ is dispensible for oxLDL uptake and foam cell formation by human and murine macrophages', Cardiovascular research, vol. 104, no. 3, pp. 467-476. https://doi.org/10.1093/cvr/cvu213

TY - JOUR

T1 - PKCδ is dispensible for oxLDL uptake and foam cell formation by human and murine macrophages

AU - Szilagyi, Katka

AU - Meijer, Alexander B.

AU - Neele, Annette E.

AU - Verkuijlen, Paul

AU - Leitges, Michael

AU - Dabernat, Sandrine

AU - Förster-Waldl, Elisabeth

AU - Boztug, Kaan

AU - Belot, Alexandre

AU - Kuijpers, Taco W.

AU - Kraal, Georg

AU - de Winther, Menno P. J.

AU - van den Berg, Timo K.

AU - Forster-Waldl, E.

PY - 2014

Y1 - 2014

N2 - Uptake of oxidized lipoprotein particles (oxLDL) and foam cell formation by macrophages is one of the first steps in the development of atherosclerosis. Recently, protein kinase C δ (PKCδ) has been implicated as a regulator of oxLDL uptake and foam cell formation via down-regulation of PKCβ and scavenger receptors CD36 and SR-A expression. Here, we describe studies in which we have re-evaluated the role of PKCδ in oxLDL uptake and foam cell formation. PKCδ expression was silenced in the human monocytic cell lines and also in primary human monocytes to analyse oxLDL uptake and CD36 expression. Additionally, bone marrow-derived macrophages of PKCδ knockout mice and macrophages cultured from patients with rare null mutations in the PRKCD gene were tested for uptake of oxLDL and foam cell formation. Expression of scavenger receptor CD36 was determined and levels of PKCβ isoforms were quantified. Neither a reduction in PKCδ levels nor its complete absence resulted in a detectable effect on the uptake of oxLDL and the formation of foam cells. PKCδ is dispensible for oxLDL uptake and foam cell formation by monocytes and macrophages

AB - Uptake of oxidized lipoprotein particles (oxLDL) and foam cell formation by macrophages is one of the first steps in the development of atherosclerosis. Recently, protein kinase C δ (PKCδ) has been implicated as a regulator of oxLDL uptake and foam cell formation via down-regulation of PKCβ and scavenger receptors CD36 and SR-A expression. Here, we describe studies in which we have re-evaluated the role of PKCδ in oxLDL uptake and foam cell formation. PKCδ expression was silenced in the human monocytic cell lines and also in primary human monocytes to analyse oxLDL uptake and CD36 expression. Additionally, bone marrow-derived macrophages of PKCδ knockout mice and macrophages cultured from patients with rare null mutations in the PRKCD gene were tested for uptake of oxLDL and foam cell formation. Expression of scavenger receptor CD36 was determined and levels of PKCβ isoforms were quantified. Neither a reduction in PKCδ levels nor its complete absence resulted in a detectable effect on the uptake of oxLDL and the formation of foam cells. PKCδ is dispensible for oxLDL uptake and foam cell formation by monocytes and macrophages

U2 - 10.1093/cvr/cvu213

DO - 10.1093/cvr/cvu213

M3 - Article

C2 - 25253077

SN - 0008-6363

VL - 104

SP - 467

EP - 476

JO - Cardiovascular research

JF - Cardiovascular research

IS - 3

ER -

PKCδ is dispensible for oxLDL uptake and foam cell formation by human and murine macrophages

Abstract

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