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Proteostasis Therapeutics representative mirna nodes
<t>Axis</t> <t>Proteostasis/homeostasis</t> and pathological protein accumulation. ( A ) Representative <t>miRNA</t> nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).
Representative Mirna Nodes, supplied by Proteostasis Therapeutics, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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Abaqus Inc ten node modified quadratic tetrahedral elements
<t>Axis</t> <t>Proteostasis/homeostasis</t> and pathological protein accumulation. ( A ) Representative <t>miRNA</t> nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).
Ten Node Modified Quadratic Tetrahedral Elements, supplied by Abaqus Inc, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/ten node modified quadratic tetrahedral elements/product/Abaqus Inc
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10X Genomics lymph node 10x visium datasets
<t>Axis</t> <t>Proteostasis/homeostasis</t> and pathological protein accumulation. ( A ) Representative <t>miRNA</t> nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).
Lymph Node 10x Visium Datasets, supplied by 10X Genomics, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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On Demand Pharmaceuticals 289 cpu node
<t>Axis</t> <t>Proteostasis/homeostasis</t> and pathological protein accumulation. ( A ) Representative <t>miRNA</t> nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).
289 Cpu Node, supplied by On Demand Pharmaceuticals, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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Huawei Technologies enterprise nodes
<t>Axis</t> <t>Proteostasis/homeostasis</t> and pathological protein accumulation. ( A ) Representative <t>miRNA</t> nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).
Enterprise Nodes, supplied by Huawei Technologies, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/enterprise nodes/product/Huawei Technologies
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Omics Data Automation sequencing node national omics data encyclopedia tss transcription start site p2g peak
<t>Axis</t> <t>Proteostasis/homeostasis</t> and pathological protein accumulation. ( A ) Representative <t>miRNA</t> nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).
Sequencing Node National Omics Data Encyclopedia Tss Transcription Start Site P2g Peak, supplied by Omics Data Automation, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/sequencing node national omics data encyclopedia tss transcription start site p2g peak/product/Omics Data Automation
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Abaqus Inc node based sub modeling technique
<t>Axis</t> <t>Proteostasis/homeostasis</t> and pathological protein accumulation. ( A ) Representative <t>miRNA</t> nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).
Node Based Sub Modeling Technique, supplied by Abaqus Inc, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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10X Genomics rna adt human lymph node dataset
<t>Axis</t> <t>Proteostasis/homeostasis</t> and pathological protein accumulation. ( A ) Representative <t>miRNA</t> nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).
Rna Adt Human Lymph Node Dataset, supplied by 10X Genomics, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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Omics Data Automation national omics data encyclopedia node
<t>Axis</t> <t>Proteostasis/homeostasis</t> and pathological protein accumulation. ( A ) Representative <t>miRNA</t> nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).
National Omics Data Encyclopedia Node, supplied by Omics Data Automation, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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Bioplus Co Ltd treatment lymph node isolates2 trim group 1 control 39 group 2 bioplus 2b
<t>Axis</t> <t>Proteostasis/homeostasis</t> and pathological protein accumulation. ( A ) Representative <t>miRNA</t> nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).
Treatment Lymph Node Isolates2 Trim Group 1 Control 39 Group 2 Bioplus 2b, supplied by Bioplus Co Ltd, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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Image Search Results


Axis Proteostasis/homeostasis and pathological protein accumulation. ( A ) Representative miRNA nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).

Journal: Metabolism Open

Article Title: Non-coding RNAs in neurodegeneration: an axis-based, evidence-tiered mechanistic synthesis

doi: 10.1016/j.metop.2026.100458

Figure Lengend Snippet: Axis Proteostasis/homeostasis and pathological protein accumulation. ( A ) Representative miRNA nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).

Article Snippet: Axis Proteostasis/homeostasis and pathological protein accumulation. ( A ) Representative miRNA nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).

Techniques:

Axis II Neuroinflammation and glia-neuron crosstalk. ( A ) miRNA axis recurrently linked to inflammatory amplification and glial activation, illustrating representative nodes associated with cytokine signaling and microglial state shifts (e.g., miR-155 and pro-inflammatory cytokine outputs; let-7a_STAT3-related signaling; miR-124 as a homeostatic regulator; and miR-195/ROCK1-linked microglial activation). ( B ) lncRNAs positioned as inflammatory “state regulators” through transcriptional and post-transcriptional control, including examples frequently discussed in neurodegenerative inflammatory contexts (e.g., MALAT1 with IL-6/TNF-α profiles; NEAT1/miR-212-3p; and TUG1/miR-152-3p/PTEN signaling). ( C ) circRNA candidates proposed to tune innate immune signaling and glial polarization, highlighting representative axes such as circ_0000518 engaging FUS/CaMKKβ/AMPK pathways and M1 polarization, and circHIPK2 acting via miRNA sequestration with downstream receptor-linked stress responses (e.g., SIGMAR1-related signaling).

Journal: Metabolism Open

Article Title: Non-coding RNAs in neurodegeneration: an axis-based, evidence-tiered mechanistic synthesis

doi: 10.1016/j.metop.2026.100458

Figure Lengend Snippet: Axis II Neuroinflammation and glia-neuron crosstalk. ( A ) miRNA axis recurrently linked to inflammatory amplification and glial activation, illustrating representative nodes associated with cytokine signaling and microglial state shifts (e.g., miR-155 and pro-inflammatory cytokine outputs; let-7a_STAT3-related signaling; miR-124 as a homeostatic regulator; and miR-195/ROCK1-linked microglial activation). ( B ) lncRNAs positioned as inflammatory “state regulators” through transcriptional and post-transcriptional control, including examples frequently discussed in neurodegenerative inflammatory contexts (e.g., MALAT1 with IL-6/TNF-α profiles; NEAT1/miR-212-3p; and TUG1/miR-152-3p/PTEN signaling). ( C ) circRNA candidates proposed to tune innate immune signaling and glial polarization, highlighting representative axes such as circ_0000518 engaging FUS/CaMKKβ/AMPK pathways and M1 polarization, and circHIPK2 acting via miRNA sequestration with downstream receptor-linked stress responses (e.g., SIGMAR1-related signaling).

Article Snippet: Axis Proteostasis/homeostasis and pathological protein accumulation. ( A ) Representative miRNA nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).

Techniques: Amplification, Activation Assay, Control

Axis IV Mitochondrial stress, oxidative injury, and autophagy-lysosome dynamics. ( A ) miRNA-linked pathways that connect mitochondrial quality control, autophagy regulation, and stress–inflammation coupling, highlighting representative nodes discussed in PD and related neurodegenerative contexts (e.g., miR-124 aligned with autophagy regulation; and miR-195/ROCK1-associated microglial activation as a mechanistic bridge between inflammation and cellular stress). ( B ) lncRNA candidates implicated in proteostasis–mitochondrial crosstalk through ubiquitination and lysosome/autophagy axis, illustrating examples such as lnc-ABCA12-3/UBQLN1-linked ubiquitination/autophagy pathways and lnc-HIBADH-4 miR-326 CTSD axes that converge on lysosomal protease activity and autophagy flux. ( C ) circRNA mediated tuning of mitochondrial homeostasis and mitophagy pathways, highlighting representative ceRNA-like motifs including circEPS15/miR-24-3p/PINK1–PRKN-dependent mitophagy, and circ016719/miR-29c/Map2k6-associated stress survival and apoptosis regulation. (For interpretation of the references to colour in this figure legend, the reader is referred to the Web version of this article.)

Journal: Metabolism Open

Article Title: Non-coding RNAs in neurodegeneration: an axis-based, evidence-tiered mechanistic synthesis

doi: 10.1016/j.metop.2026.100458

Figure Lengend Snippet: Axis IV Mitochondrial stress, oxidative injury, and autophagy-lysosome dynamics. ( A ) miRNA-linked pathways that connect mitochondrial quality control, autophagy regulation, and stress–inflammation coupling, highlighting representative nodes discussed in PD and related neurodegenerative contexts (e.g., miR-124 aligned with autophagy regulation; and miR-195/ROCK1-associated microglial activation as a mechanistic bridge between inflammation and cellular stress). ( B ) lncRNA candidates implicated in proteostasis–mitochondrial crosstalk through ubiquitination and lysosome/autophagy axis, illustrating examples such as lnc-ABCA12-3/UBQLN1-linked ubiquitination/autophagy pathways and lnc-HIBADH-4 miR-326 CTSD axes that converge on lysosomal protease activity and autophagy flux. ( C ) circRNA mediated tuning of mitochondrial homeostasis and mitophagy pathways, highlighting representative ceRNA-like motifs including circEPS15/miR-24-3p/PINK1–PRKN-dependent mitophagy, and circ016719/miR-29c/Map2k6-associated stress survival and apoptosis regulation. (For interpretation of the references to colour in this figure legend, the reader is referred to the Web version of this article.)

Article Snippet: Axis Proteostasis/homeostasis and pathological protein accumulation. ( A ) Representative miRNA nodes implicated in proteostasis collapse across neurodegenerative settings, highlighting links to amyloidogenic processing and stress signaling (e.g., miR-29/BACE1 in Aβ plaque burden; miR-146a–NF-κB signaling intersecting with tau-related pathology; and ALS-associated vulnerability aligned with impaired miRNA processing such as miR-218 depletion). ( B ) lncRNA-mediated regulation of proteostasis-related gene axis, emphasizing lncRNAs proposed to modulate amyloidogenic pathways and protein handling (e.g., BACE1-AS, NDM29, and 51A/SORL1-related mechanisms), as well as aggregation-relevant nodes reported in PD contexts (e.g., HOTAIR–miR-221-3p–α-synuclein-related phenotypes). ( C ) circRNA-linked regulatory motifs that converge on neuronal injury and proteostasis-adjacent clearance pathways, primarily via miRNA-coupled axes (e.g., circAXL/miR-328/BACE1; circLPAR1/miR-212-3p/ZNF217; and circBptf/miR-138-5p/p62/SQSTM1).

Techniques: Control, Activation Assay, Ubiquitin Proteomics, Activity Assay