Hyperthermic induction of the 27-kDa heat shock protein (Hsp27) in neuroglia and neurons of the rat central nervous system

Krueger-Naug, Anne Marie R.; Hopkins, David A.; Armstrong, John N.; Plumier, Jean Christophe; Currie, R. William

doi:10.1002/1096-9861(20001218)428:3<495::aid-cne7>3.0.co;2-4

Cited by 53 publications

(33 citation statements)

References 70 publications

(88 reference statements)

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“…After hyperthermic treatment, select neurons of the hippocampal formation, of the hypothalamus, such as paraventricular nucleus and dorsomedial hypothalamic nucleus, and of the circumventricular organs, such as subfornical organ and area postrema, expressed high levels of Hsp27. This suggests that some Hsp27-positive cells are involved in physiological responses to body fluid homeostasis (Krueger-Naug et al 2000). In addition, these regions of the brain are involved in the modulation of blood pressure by Ang II (Lenkei et al 1997).…”

Section: Discussionmentioning

confidence: 99%

Heat shock treatment protects against angiotensin II–induced hypertension and inflammation in aorta

Chen

Ross²,

Currie³

2004

Cell Stress Chaperones

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Angiotensin II (Ang II) is a potent vasoconstrictor and induces inflammation and end-organ injury through its activation of the proinflammatory transcription factor, nuclear factor-B (NF-B). Heat shock (HS) treatment with subsequent expression of heat shock proteins (Hsps) is an effective strategy for tissue protection against oxidative injuries. Recently, HS and Hsps have been shown to interact with NF-B in tissue injury. In this study, we investigated whether HS could protect against Ang II-induced hypertension and inflammation by inhibiting NF-B. Sprague-Dawley rats were divided into control and HS groups. Control and 24-hour post-heat shocked rats were treated with Ang II. At days 1, 3, 5, 7, 11, and 14 after Ang II administration, systolic blood pressures were measured by tail-cuff plethysmography, and aorta tissues were collected. Aorta NF-B deoxyribonucleic acid-binding activity was measured by electrophoretic mobility shift assay, and NF-B p65 subunit, Hsp70, Hsp27, and interleukin-6 (IL-6) expressions were measured by Western analysis. HS treatment significantly decreased Ang II-induced hypertension. The activation of NF-B in aorta by Ang II was suppressed by HS treatment. The elevated expression of IL-6 induced by Ang II treatment was also decreased by HS treatment. Although Ang II treatment induced an increase in Hsp70 and Hsp27, HS treatment induced a greater elevation of Hsp70 and Hsp27 expression. HS treatment protects against Ang II-induced hypertension and inflammation. This protection may relate to the interaction of Hsps and the NF-B pathway.

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Section: Discussionmentioning

confidence: 99%

Heat shock treatment protects against angiotensin II–induced hypertension and inflammation in aorta

Chen

Ross²,

Currie³

2004

Cell Stress Chaperones

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“…Sections were incubated with phosphate-buffered saline (PBS) containing 0.1% Triton-X (PBS-X) and 10% goat serum for 1 h at room temperature. Primary rabbit polyclonal antibody specific for the murine 25 kDa heat shock protein, Hsp25, and the homologous rat Hsp27 (Plumier et al, 1997c;Krueger-Naug et al, 2000, 2002aArmstrong et al, 2001; StressGen Biotechnologies Corporation, Victoria, BC, Canada) was diluted 1:1000 in PBS-X with 2% goat serum and incubated overnight at 4°C. After three 10-min rinses, sections were incubated for 3 h in PBS (no Triton-X) containing Alexa goat anti-rabbit 546 (1:500; Molecular Probes, Eugene, OR, USA).…”

Section: Immunohistochemistrymentioning

confidence: 99%

“…In the peripheral nervous system, sciatic nerve injury and vagotomy have resulted in the induction and prolonged expression of Hsp27 in the affected neurons (Costigan et al, 1998;Hopkins et al, 1998;Lewis et al, 1999). Hyperthermia causes the induction of Hsp27 primarily in astroglia throughout the CNS; in addition, hyperthermia results in Hsp27 expression in specific nuclei associated with fluid homeostasis and thermoregulation (Krueger-Naug et al, 2000). With excitotoxic injury such as kainic acid-induced status epilepticus (Plumier et al, 1996), and potassium chloride-induced cortical spreading depression (Plumier et al, 1997b), Hsp27 is detected primarily in astrocytes.…”

Section: Cell Type-specific and Stress-dependent Expression Of Hsp27mentioning

confidence: 99%

Administration of brain-derived neurotrophic factor suppresses the expression of heat shock protein 27 in rat retinal ganglion cells following axotomy

et al. 2003

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“…For example, transient ischemia and subsequent reperfusion of rat CP markedly attenuate Na + /K + -ATPase activity and the capacity for glutamate accumulation (Ennis and Keep, 2006;Johanson et al, 2000;Palm et al, 1995). However, this brain barrier mounts a cellular stress response (Blake et al, 1990;Brown, 1991;Krueger-Naug et al, 2000), which in other tissues can be generally protective against physicochemical stressors such as ischemia, hyperthermia, oxidants or heavy metals and may ameliorate loss of function in CP.…”

Section: Introductionmentioning

confidence: 99%

Trimethylamine oxide suppresses stress-induced alteration of organic anion transport in choroid plexus

Villalobos

Renfro

2007

Journal of Experimental Biology

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Zn for 6·h induced a twofold greater Hsp70 accumulation in the absence of TMAO than in its presence, and the higher Hsp70 level was associated with a higher 2,4-D transport rate. Heat stress and 50·mol·l -1 Zn also induced more pronounced increases in Hsp70 mRNA in the absence of TMAO. Thus, the cellular stress response can significantly alter CP organic anion transport capacity, and an endogenous osmolyte can suppress that response.

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Hyperthermic induction of the 27-kDa heat shock protein (Hsp27) in neuroglia and neurons of the rat central nervous system

Cited by 53 publications

References 70 publications

Heat shock treatment protects against angiotensin II–induced hypertension and inflammation in aorta

Heat shock treatment protects against angiotensin II–induced hypertension and inflammation in aorta

Administration of brain-derived neurotrophic factor suppresses the expression of heat shock protein 27 in rat retinal ganglion cells following axotomy

Trimethylamine oxide suppresses stress-induced alteration of organic anion transport in choroid plexus

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