RETRACTED ARTICLE: Treatment with a brain-selective prodrug of 17β-estradiol improves cognitive function in Alzheimer’s disease mice by regulating klf5-NF-κB pathway

Yan, Wenhao; Wu, Jun; Song, Bo; Luo, Qiang; Xu, Yuming

doi:10.1007/s00210-019-01639-w

Cited by 12 publications

(10 citation statements)

References 34 publications

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“…Thus far, DHED (Figure 3B) has been studied most extensively in preclinical animal models of E2-responsive maladies [23,36,50,51]. The unprecedented CNS selectivity of our approach in terms of prodrug bioactivation has also recently been confirmed independently from our laboratory [52,53]. We have also unambiguously shown the CNS-selective bioactivations of HEDD and αDHD to E1 and αE2, respectively [35,37].…”

Section: Bioprecursor Prodrugs For Cns-selective Estrogen Therapysupporting

confidence: 69%

“…Consequently, these animals had a higher cognitive performance, similar to those treated with the parent E2, when compared to the untreated control group. An independent follow-up study not only have confirmed these promising results, but also found that DHED treatment reduced oxidative and inflammatory stress, as well as decreased phosphorylated tau (τ) protein levels in OVX transgenic AD mouse [52]. An investigation focusing on assessing DHED’s therapeutic potential in males of the APPswe/PS1dE9 DTG-mouse AD model also revealed reduction of Aβ formation and protection against Aβ-associated cognitive impairment, as summarized in Figure 7 [51].…”

Section: Bioprecursor Prodrugs For Cns-selective Estrogen Therapymentioning

confidence: 86%

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A Novel Prodrug Approach for Central Nervous System-Selective Estrogen Therapy

Prókai-Tátrai

Prókai

2019

Molecules

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Beneficial effects of estrogens in the central nervous system (CNS) results from the synergistic combination of their well-orchestrated genomic and non-genomic actions, making them potential broad-spectrum neurotherapeutic agents. However, owing to unwanted peripheral hormonal burdens by any currently known non-invasive drug administrations, the development of estrogens as safe pharmacotherapeutic modalities cannot be realized until they are confined specifically and selectively to the site of action. We have developed small-molecule bioprecursor prodrugs carrying the para-quinol scaffold on the steroidal A-ring that are preferentially metabolized in the CNS to the corresponding estrogens. Here, we give an overview of our discovery of these prodrugs. Selected examples are shown to illustrate that, independently of the route of administrations and duration of treatments, these agents produce high concentration of estrogens only in the CNS without peripheral hormonal liability. 10β,17β-Dihydroxyestra-1,4-dien-3-one (DHED) has been the best-studied representative of this novel type of prodrugs for brain and retina health. Specific applications in preclinical animal models of centrally-regulated and estrogen-responsive human diseases, including neurodegeneration, menopausal symptoms, cognitive decline and depression, are discussed to demonstrate the translational potential of our prodrug approach for CNS-selective and gender-independent estrogen therapy with inherent therapeutic safety.

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Section: Bioprecursor Prodrugs For Cns-selective Estrogen Therapysupporting

confidence: 69%

Section: Bioprecursor Prodrugs For Cns-selective Estrogen Therapymentioning

confidence: 86%

A Novel Prodrug Approach for Central Nervous System-Selective Estrogen Therapy

Prókai-Tátrai

Prókai

2019

Molecules

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“…Notably, THAP1 has been observed to have a binding site in the specificity protein 1 (Sp1) promoter in humans 31 , and Sp1 was reported to be enriched for binding motifs in AD hyperacetylated peaks in Marzi et al (2018). Amongst microglia-specific and oligodendrocyte-specific AD hyperacetylated peaks we observed significant enrichment of binding motifs for Krüppel-like transcription factor 5 (KLF5) (microglia: P < 1 × 10 −16 , oligodendrocytes: P < 1 × 10 −91 ), a transcription factor implicated in inflammatory responses 32 .…”

Section: Resultsmentioning

confidence: 98%

CHAS, a deconvolution tool, infers cell type-specific signatures in bulk brain histone acetylation studies of neurological and psychiatric disorders

Murphy

Nott

Marzi

2021

Preprint

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Chromatin profiling studies have shown the importance of gene regulation in driving heritability and environmental risk of brain disorders. Acetylation of histone H3 lysine 27 (H3K27ac) has emerged as an informative disease-associated epigenetic mark. However, cell type-specific contributions to epigenetic dysregulation in disease are unclear as studies have often used bulk brain tissue. Therefore, methods for the deconvolution of bulk H3K27ac profiles are critical. Here we developed the Cell type-specific Histone Acetylation Score (CHAS), a computational tool for inferring cell type-specific signatures in bulk brain H3K27ac profiles. CHAS annotates peaks identified in bulk brain studies of H3K27ac to cell type-specific signals in four major brain cell types, and derives cell type-specific histone acetylation scores as a proxy for cell type proportion. Our method was validated in pseudo-bulk samples and applied to three brain disorder epigenome-wide association studies conducted on bulk brain tissue. CHAS exposed shifts in cellular proportions in Alzheimer's disease (AD), in line with neuropathology, and identified disrupted gene regulatory elements in oligodendrocytes in AD and microglia in autism spectrum disorder (ASD). This contrasts with heritability-based enrichment analyses which indicate genetic risk is associated with microglia in AD and neurons in ASD. Our approach identified cell type specific signalling pathways and putative upstream transcription factors associated with these elements. CHAS enables deconvolution of H3K27ac in bulk brain tissue, yielding cell type-specific biological insights into brain disease-associated regulatory variation.

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“…Moreover, sex hormones were known to influence kidney disease 62 . It was reported that androgen‐induced KLF5 expression in human breast cancer cell lines and a prodrug of 17β‐oestradiol inhibited KLF5‐NFκB inflammatory pathway in the Alzheimer's Disease mouse model 63,64 . In addition, oncogenic regulator protein SET inhibited KLF5 activation by binding to its DNA‐binding domain (DBD).…”

Section: Post‐translational Transcriptional Post‐transcriptional Rementioning

confidence: 99%

Roles of Krüppel‐like factor 5 in kidney disease

Liu

Zhou

et al. 2021

J Cellular Molecular Medi

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Transcription factor Krüppel‐like factor 5 (KLF5) is a member of the Krüppel‐like factors’ (KLFs) family. KLF5 regulates a number of cellular functions, such as apoptosis, proliferation and differentiation. Therefore, KLF5 can play a role in many diseases, including, cancer, cardiovascular disease and gastrointestinal disorders. An important role for KLF5 in the kidney was recently reported, such that KLF5 regulated podocyte apoptosis, renal cell proliferation, tubulointerstitial inflammation and renal fibrosis. In this review, we have summarized the available information in the literature with a brief description on how transcriptional, post‐transcriptional and post‐translational modifications of KLF5 modulate its function in a variety of organs including the kidney with a focus of its importance on the pathogenesis of various kidney diseases. Furthermore, we also have outlined the current and possible mechanisms of KLF5 activation in kidney diseases. These studies suggest a need for more systemic investigations, particularly for generation of animal models with renal cell‐specific deletion or overexpression of KLF5 gene to examine direct contributions of KLF5 to various kidney diseases. This will promote further experimentation in the development of therapies to prevent or treat various kidney diseases.

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RETRACTED ARTICLE: Treatment with a brain-selective prodrug of 17β-estradiol improves cognitive function in Alzheimer’s disease mice by regulating klf5-NF-κB pathway

Cited by 12 publications

References 34 publications

A Novel Prodrug Approach for Central Nervous System-Selective Estrogen Therapy

A Novel Prodrug Approach for Central Nervous System-Selective Estrogen Therapy

CHAS, a deconvolution tool, infers cell type-specific signatures in bulk brain histone acetylation studies of neurological and psychiatric disorders

Roles of Krüppel‐like factor 5 in kidney disease

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