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PD-1/PD-L1 checkpoint blockade harnesses monocyte-derived macrophages to combat cognitive impairment in a tauopathy mouse model

Blocking the PD-1 pathway was shown to be effective in amyloid beta mouse models, yet little is known about its therapeutic potential in models of tauopathy. The authors show here that blocking PD-L1, a PD-1 ligand, is similarly effective, and that both treatments reversed cognitive deficiencies, and modified disease pathology not only in an animal model of AD, but also in the DM-hTAU mouse tauopathy model, through a mechanism that involves monocyte-derived macrophages.

Neta Rosenzweig
Raz Dvir-Szternfeld
Michal Schwartz
ResearchOpen Access28 Jan 2019
Nature Communications

Volume: 10, P: 1-15
Breaking immune tolerance by targeting Foxp3⁺ regulatory T cells mitigates Alzheimer’s disease pathology

Immunosuppression has been unsuccessful in treatment of Alzheimer’s disease. Here the authors show in a mouse model of the disease that transient inhibition of regulatory T cells mitigates amyloid plaque pathology and reverses cognitive decline, whereas augmenting these cells worsens the pathology.

Kuti Baruch
Neta Rosenzweig
Michal Schwartz
ResearchOpen Access18 Aug 2015
Nature Communications

Volume: 6, P: 1-12
The 8q24 cancer risk variant rs6983267 shows long-range interaction with MYC in colorectal cancer

Matthew Freedman and colleagues show that a region on 8q24 associated with colorectal cancer risk functions as an enhancer and undergoes long-range interactions with MYC. They further show that alleles at the risk-associated SNP bind differentially to TCF7L2, a transcription factor in the Wnt pathway.

Mark M Pomerantz
Nasim Ahmadiyeh
Matthew L Freedman
Research28 Jun 2009
Nature Genetics

Volume: 41, P: 882-884
RUNX1 prevents oestrogen-mediated AXIN1 suppression and β-catenin activation in ER-positive breast cancer

The tumour suppressor RUNX1 is often lost or mutated in oestrogen receptor-positive breast cancers. In this study, the authors demonstrate that the loss of RUNX1 unleashes oestrogen-mediated inhibition of AXIN1, a negative regulator of β-catenin, resulting in β-catenin signalling-mediated cancer cell proliferation and mitosis deregulation.

Nyam-Osor Chimge
Gillian H. Little
Baruch Frenkel
ResearchOpen Access26 Feb 2016
Nature Communications

Volume: 7, P: 1-12
Alterations in Brca1 expression in mouse ovarian granulosa cells have short-term and long-term consequences on estrogen-responsive organs

Hai-Yun Yen
Yankel Gabet
Louis Dubeau
Research09 Apr 2012
Laboratory Investigation

Volume: 92, P: 802-811

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PD-1/PD-L1 checkpoint blockade harnesses monocyte-derived macrophages to combat cognitive impairment in a tauopathy mouse model

Breaking immune tolerance by targeting Foxp3⁺ regulatory T cells mitigates Alzheimer’s disease pathology

The 8q24 cancer risk variant rs6983267 shows long-range interaction with MYC in colorectal cancer

RUNX1 prevents oestrogen-mediated AXIN1 suppression and β-catenin activation in ER-positive breast cancer

Alterations in Brca1 expression in mouse ovarian granulosa cells have short-term and long-term consequences on estrogen-responsive organs

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PD-1/PD-L1 checkpoint blockade harnesses monocyte-derived macrophages to combat cognitive impairment in a tauopathy mouse model

Breaking immune tolerance by targeting Foxp3+ regulatory T cells mitigates Alzheimer’s disease pathology

The 8q24 cancer risk variant rs6983267 shows long-range interaction with MYC in colorectal cancer

RUNX1 prevents oestrogen-mediated AXIN1 suppression and β-catenin activation in ER-positive breast cancer

Alterations in Brca1 expression in mouse ovarian granulosa cells have short-term and long-term consequences on estrogen-responsive organs

Search

Quick links

Breaking immune tolerance by targeting Foxp3⁺ regulatory T cells mitigates Alzheimer’s disease pathology