Activated protein C therapy slows ALS-like disease in mice by transcriptionally inhibiting SOD1 in motor neurons and microglia cells
Zhihui Zhong, … , Don W. Cleveland, Berislav V. Zlokovic
Zhihui Zhong, … , Don W. Cleveland, Berislav V. Zlokovic
Published October 19, 2009
Citation Information: J Clin Invest. 2009;119(11):3437-3449. https://doi.org/10.1172/JCI38476.
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Research Article

Activated protein C therapy slows ALS-like disease in mice by transcriptionally inhibiting SOD1 in motor neurons and microglia cells

Abstract

Activated protein C (APC) is a signaling protease with anticoagulant activity. Here, we have used mice expressing a mutation in superoxide dismutase-1 (SOD1) that is linked to amyotrophic lateral sclerosis (ALS) to show that administration of APC or APC analogs with reduced anticoagulant activity after disease onset slows disease progression and extends survival. A proteolytically inactive form of APC with reduced anticoagulant activity provided no benefit. APC crossed the blood–spinal cord barrier in mice via endothelial protein C receptor. When administered after disease onset, APC eliminated leakage of hemoglobin-derived products across the blood–spinal cord barrier and delayed microglial activation. In microvessels, motor neurons, and microglial cells from SOD1-mutant mice and in cultured neuronal cells, APC transcriptionally downregulated SOD1. Inhibition of SOD1 synthesis in neuronal cells by APC required protease-activated receptor–1 (PAR1) and PAR3, which inhibited nuclear transport of the Sp1 transcription factor. Diminished mutant SOD1 synthesis by selective gene excision within endothelial cells did not alter disease progression, which suggests that diminished mutant SOD1 synthesis in other cells, including motor neurons and microglia, caused the APC-mediated slowing of disease. The delayed disease progression in mice after APC administration suggests that this approach may be of benefit to patients with familial, and possibly sporadic, ALS.

Authors

Zhihui Zhong, Hristelina Ilieva, Lee Hallagan, Robert Bell, Itender Singh, Nicole Paquette, Meenakshisundaram Thiyagarajan, Rashid Deane, Jose A. Fernandez, Steven Lane, Anna B. Zlokovic, Todd Liu, John H. Griffin, Nienwen Chow, Francis J. Castellino, Konstantin Stojanovic, Don W. Cleveland, Berislav V. Zlokovic

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Figure 9

5A-APC–mediated SOD1 downregulation in motor neurons and spinal cord endothelium requires endothelial EPCR.

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5A-APC–mediated SOD1 downregulation in motor neurons and spinal cord end...
(AC) mSOD1 mRNA levels, determined by QPCR (A), and immunoblotting (B) and densitometry analysis (C) of mSOD1 protein, in laser-captured motor neurons from EPCRδ/δ and EPCR+/+ mice treated with saline or 100 μg/kg/d 5A-APC i.p. for 7 days. (DF) mSOD1 mRNA levels (D), and immunoblotting (E) and densitometry (F) analysis of mSOD1 protein levels, in spinal cord microvessels isolated from EPCRδ/δ and EPCR+/+ mice treated as in AC. (AF) n = 3–4 per group. (GI) SOD1G93A and mSOD1 mRNA levels (G), and immunoblotting (H) and densitometry (I) analysis of SOD1G93A and mSOD1 protein levels, in laser-captured spinal cord motor neurons of SOD1G93A mice treated with saline or 100 μg/kg/d 5A-APC i.p. for 7 days in the absence or presence of an EPCR blocking antibody (RCR-252) or nonimmune IgG infused through the femoral vein (40 μg/mouse) at day 1 and 3. (JL) SOD1G93A and mSOD1 mRNA levels (J), and immunoblotting (K) and densitometry (L) analysis of SOD1G93A and mSOD1 protein levels, in spinal cord microvessels isolated from SOD1G93A mice treated as in GI. (GL) n = 3–5.