PubMed:30630951 JSONTXT

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    Glycosmos15-CL

    {"project":"Glycosmos15-CL","denotations":[{"id":"T1","span":{"begin":935,"end":948},"obj":"Cell"}],"attributes":[{"id":"A1","pred":"cl_id","subj":"T1","obj":"http://purl.obolibrary.org/obo/CL:0000100"}],"text":"Aggregation of the nucleic acid-binding protein TDP-43 occurs via distinct routes that are coordinated with stress granule formation.\nTAR DNA-binding protein 43 (TDP-43) is a nucleic acid-binding protein, and its aggregation represents the defining pathology in amyotrophic lateral sclerosis (ALS) and related proteinopathies. Recent studies implicate cytoplasmic stress granules (SGs) as hubs that may facilitate TDP-43 aggregation. Here, using cellular fractionation, biochemical analyses, and histological assays, we show that TDP-43 targeted to the cytoplasm has multiple fates. Whereas a TDP-43 subpopulation is indeed recruited to SGs, mature aggregated TDP-43, produced with aggregate-prone TDP-43 variants or exposure to oxidative stress, generates distinct TDP-43 inclusions that are surprisingly devoid of SGs. Consistent with this observation, we found that SG components are predominantly excluded from TDP-43 pathology in motor neurons from individuals with ALS. We generated de novo SGs by expressing the fragile X protein (FMRP) and found that rather than directly engaging TDP-43 aggregates, SGs can sequester the proteostasis factor histone deacetylase 6 (HDAC6) and thereby impede TDP-43 clearance from cells. These findings indicate that SGs form distinct cytoplasmic structures that can indirectly enhance TDP-43 aggregation. Therapeutic approaches that inhibit SG formation may therefore be effective at suppressing TDP-43-mediated toxicity in patients with ALS and related TDP-43 proteinopathies."}

    PubMed_ArguminSci

    {"project":"PubMed_ArguminSci","denotations":[{"id":"T1","span":{"begin":134,"end":326},"obj":"DRI_Background"},{"id":"T2","span":{"begin":327,"end":433},"obj":"DRI_Background"},{"id":"T3","span":{"begin":434,"end":582},"obj":"DRI_Background"},{"id":"T4","span":{"begin":583,"end":681},"obj":"DRI_Background"},{"id":"T5","span":{"begin":705,"end":820},"obj":"DRI_Background"},{"id":"T6","span":{"begin":821,"end":975},"obj":"DRI_Outcome"},{"id":"T7","span":{"begin":976,"end":1227},"obj":"DRI_Approach"},{"id":"T8","span":{"begin":1228,"end":1345},"obj":"DRI_Background"},{"id":"T9","span":{"begin":1346,"end":1494},"obj":"DRI_Background"},{"id":"T10","span":{"begin":1517,"end":1518},"obj":"DRI_Background"}],"text":"Aggregation of the nucleic acid-binding protein TDP-43 occurs via distinct routes that are coordinated with stress granule formation.\nTAR DNA-binding protein 43 (TDP-43) is a nucleic acid-binding protein, and its aggregation represents the defining pathology in amyotrophic lateral sclerosis (ALS) and related proteinopathies. Recent studies implicate cytoplasmic stress granules (SGs) as hubs that may facilitate TDP-43 aggregation. Here, using cellular fractionation, biochemical analyses, and histological assays, we show that TDP-43 targeted to the cytoplasm has multiple fates. Whereas a TDP-43 subpopulation is indeed recruited to SGs, mature aggregated TDP-43, produced with aggregate-prone TDP-43 variants or exposure to oxidative stress, generates distinct TDP-43 inclusions that are surprisingly devoid of SGs. Consistent with this observation, we found that SG components are predominantly excluded from TDP-43 pathology in motor neurons from individuals with ALS. We generated de novo SGs by expressing the fragile X protein (FMRP) and found that rather than directly engaging TDP-43 aggregates, SGs can sequester the proteostasis factor histone deacetylase 6 (HDAC6) and thereby impede TDP-43 clearance from cells. These findings indicate that SGs form distinct cytoplasmic structures that can indirectly enhance TDP-43 aggregation. Therapeutic approaches that inhibit SG formation may therefore be effective at suppressing TDP-43-mediated toxicity in patients with ALS and related TDP-43 proteinopathies."}

    Goldhamster2_Cellosaurus

    {"project":"Goldhamster2_Cellosaurus","denotations":[{"id":"T1","span":{"begin":52,"end":54},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T2","span":{"begin":134,"end":137},"obj":"CVCL_WI26|Cancer_cell_line|Homo sapiens"},{"id":"T3","span":{"begin":158,"end":160},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T4","span":{"begin":166,"end":168},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T5","span":{"begin":173,"end":174},"obj":"CVCL_6479|Finite_cell_line|Mus musculus"},{"id":"T6","span":{"begin":381,"end":384},"obj":"CVCL_4007|Cancer_cell_line|Rattus norvegicus"},{"id":"T7","span":{"begin":399,"end":402},"obj":"CVCL_E773|Transformed_cell_line|Homo sapiens"},{"id":"T8","span":{"begin":418,"end":420},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T9","span":{"begin":517,"end":519},"obj":"CVCL_5M23|Cancer_cell_line|Mesocricetus auratus"},{"id":"T10","span":{"begin":534,"end":536},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T11","span":{"begin":563,"end":566},"obj":"CVCL_6758|Undefined_cell_line_type|Cricetulus griseus"},{"id":"T12","span":{"begin":563,"end":566},"obj":"CVCL_E689|Transformed_cell_line|Homo sapiens"},{"id":"T13","span":{"begin":591,"end":592},"obj":"CVCL_6479|Finite_cell_line|Mus musculus"},{"id":"T14","span":{"begin":597,"end":599},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T15","span":{"begin":637,"end":640},"obj":"CVCL_4007|Cancer_cell_line|Rattus norvegicus"},{"id":"T16","span":{"begin":664,"end":666},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T17","span":{"begin":702,"end":704},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T18","span":{"begin":770,"end":772},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T19","span":{"begin":816,"end":819},"obj":"CVCL_4007|Cancer_cell_line|Rattus norvegicus"},{"id":"T20","span":{"begin":855,"end":857},"obj":"CVCL_5M23|Cancer_cell_line|Mesocricetus auratus"},{"id":"T21","span":{"begin":869,"end":871},"obj":"CVCL_IP74|Cancer_cell_line|Homo sapiens"},{"id":"T22","span":{"begin":869,"end":871},"obj":"CVCL_M617|Cancer_cell_line|Homo sapiens"},{"id":"T23","span":{"begin":919,"end":921},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T24","span":{"begin":976,"end":978},"obj":"CVCL_5M23|Cancer_cell_line|Mesocricetus auratus"},{"id":"T25","span":{"begin":997,"end":1000},"obj":"CVCL_4007|Cancer_cell_line|Rattus norvegicus"},{"id":"T26","span":{"begin":1093,"end":1095},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T27","span":{"begin":1108,"end":1111},"obj":"CVCL_4007|Cancer_cell_line|Rattus norvegicus"},{"id":"T28","span":{"begin":1203,"end":1205},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T29","span":{"begin":1257,"end":1260},"obj":"CVCL_4007|Cancer_cell_line|Rattus norvegicus"},{"id":"T30","span":{"begin":1330,"end":1332},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T31","span":{"begin":1382,"end":1384},"obj":"CVCL_IP74|Cancer_cell_line|Homo sapiens"},{"id":"T32","span":{"begin":1382,"end":1384},"obj":"CVCL_M617|Cancer_cell_line|Homo sapiens"},{"id":"T33","span":{"begin":1395,"end":1398},"obj":"CVCL_E773|Transformed_cell_line|Homo sapiens"},{"id":"T34","span":{"begin":1441,"end":1443},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"},{"id":"T35","span":{"begin":1499,"end":1501},"obj":"CVCL_UU94|Spontaneously_immortalized_cell_line|Cricetulus griseus"}],"text":"Aggregation of the nucleic acid-binding protein TDP-43 occurs via distinct routes that are coordinated with stress granule formation.\nTAR DNA-binding protein 43 (TDP-43) is a nucleic acid-binding protein, and its aggregation represents the defining pathology in amyotrophic lateral sclerosis (ALS) and related proteinopathies. Recent studies implicate cytoplasmic stress granules (SGs) as hubs that may facilitate TDP-43 aggregation. Here, using cellular fractionation, biochemical analyses, and histological assays, we show that TDP-43 targeted to the cytoplasm has multiple fates. Whereas a TDP-43 subpopulation is indeed recruited to SGs, mature aggregated TDP-43, produced with aggregate-prone TDP-43 variants or exposure to oxidative stress, generates distinct TDP-43 inclusions that are surprisingly devoid of SGs. Consistent with this observation, we found that SG components are predominantly excluded from TDP-43 pathology in motor neurons from individuals with ALS. We generated de novo SGs by expressing the fragile X protein (FMRP) and found that rather than directly engaging TDP-43 aggregates, SGs can sequester the proteostasis factor histone deacetylase 6 (HDAC6) and thereby impede TDP-43 clearance from cells. These findings indicate that SGs form distinct cytoplasmic structures that can indirectly enhance TDP-43 aggregation. Therapeutic approaches that inhibit SG formation may therefore be effective at suppressing TDP-43-mediated toxicity in patients with ALS and related TDP-43 proteinopathies."}

    GoldHamster

    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Recent studies implicate cytoplasmic stress granules (SGs) as hubs that may facilitate TDP-43 aggregation. Here, using cellular fractionation, biochemical analyses, and histological assays, we show that TDP-43 targeted to the cytoplasm has multiple fates. Whereas a TDP-43 subpopulation is indeed recruited to SGs, mature aggregated TDP-43, produced with aggregate-prone TDP-43 variants or exposure to oxidative stress, generates distinct TDP-43 inclusions that are surprisingly devoid of SGs. Consistent with this observation, we found that SG components are predominantly excluded from TDP-43 pathology in motor neurons from individuals with ALS. We generated de novo SGs by expressing the fragile X protein (FMRP) and found that rather than directly engaging TDP-43 aggregates, SGs can sequester the proteostasis factor histone deacetylase 6 (HDAC6) and thereby impede TDP-43 clearance from cells. These findings indicate that SGs form distinct cytoplasmic structures that can indirectly enhance TDP-43 aggregation. Therapeutic approaches that inhibit SG formation may therefore be effective at suppressing TDP-43-mediated toxicity in patients with ALS and related TDP-43 proteinopathies."}

    sentences

    {"project":"sentences","denotations":[{"id":"T1","span":{"begin":0,"end":133},"obj":"Sentence"},{"id":"T2","span":{"begin":134,"end":326},"obj":"Sentence"},{"id":"T3","span":{"begin":327,"end":433},"obj":"Sentence"},{"id":"T4","span":{"begin":434,"end":582},"obj":"Sentence"},{"id":"T5","span":{"begin":583,"end":820},"obj":"Sentence"},{"id":"T6","span":{"begin":821,"end":975},"obj":"Sentence"},{"id":"T7","span":{"begin":976,"end":1227},"obj":"Sentence"},{"id":"T8","span":{"begin":1228,"end":1345},"obj":"Sentence"},{"id":"T9","span":{"begin":1346,"end":1518},"obj":"Sentence"}],"namespaces":[{"prefix":"_base","uri":"http://pubannotation.org/ontology/tao.owl#"}],"text":"Aggregation of the nucleic acid-binding protein TDP-43 occurs via distinct routes that are coordinated with stress granule formation.\nTAR DNA-binding protein 43 (TDP-43) is a nucleic acid-binding protein, and its aggregation represents the defining pathology in amyotrophic lateral sclerosis (ALS) and related proteinopathies. Recent studies implicate cytoplasmic stress granules (SGs) as hubs that may facilitate TDP-43 aggregation. Here, using cellular fractionation, biochemical analyses, and histological assays, we show that TDP-43 targeted to the cytoplasm has multiple fates. Whereas a TDP-43 subpopulation is indeed recruited to SGs, mature aggregated TDP-43, produced with aggregate-prone TDP-43 variants or exposure to oxidative stress, generates distinct TDP-43 inclusions that are surprisingly devoid of SGs. Consistent with this observation, we found that SG components are predominantly excluded from TDP-43 pathology in motor neurons from individuals with ALS. We generated de novo SGs by expressing the fragile X protein (FMRP) and found that rather than directly engaging TDP-43 aggregates, SGs can sequester the proteostasis factor histone deacetylase 6 (HDAC6) and thereby impede TDP-43 clearance from cells. These findings indicate that SGs form distinct cytoplasmic structures that can indirectly enhance TDP-43 aggregation. Therapeutic approaches that inhibit SG formation may therefore be effective at suppressing TDP-43-mediated toxicity in patients with ALS and related TDP-43 proteinopathies."}

    Glycosmos6-MAT

    {"project":"Glycosmos6-MAT","denotations":[{"id":"T1","span":{"begin":274,"end":281},"obj":"http://purl.obolibrary.org/obo/MAT_0000488"}],"text":"Aggregation of the nucleic acid-binding protein TDP-43 occurs via distinct routes that are coordinated with stress granule formation.\nTAR DNA-binding protein 43 (TDP-43) is a nucleic acid-binding protein, and its aggregation represents the defining pathology in amyotrophic lateral sclerosis (ALS) and related proteinopathies. Recent studies implicate cytoplasmic stress granules (SGs) as hubs that may facilitate TDP-43 aggregation. Here, using cellular fractionation, biochemical analyses, and histological assays, we show that TDP-43 targeted to the cytoplasm has multiple fates. Whereas a TDP-43 subpopulation is indeed recruited to SGs, mature aggregated TDP-43, produced with aggregate-prone TDP-43 variants or exposure to oxidative stress, generates distinct TDP-43 inclusions that are surprisingly devoid of SGs. Consistent with this observation, we found that SG components are predominantly excluded from TDP-43 pathology in motor neurons from individuals with ALS. We generated de novo SGs by expressing the fragile X protein (FMRP) and found that rather than directly engaging TDP-43 aggregates, SGs can sequester the proteostasis factor histone deacetylase 6 (HDAC6) and thereby impede TDP-43 clearance from cells. These findings indicate that SGs form distinct cytoplasmic structures that can indirectly enhance TDP-43 aggregation. Therapeutic approaches that inhibit SG formation may therefore be effective at suppressing TDP-43-mediated toxicity in patients with ALS and related TDP-43 proteinopathies."}

    GlyCosmos15-HP

    {"project":"GlyCosmos15-HP","denotations":[{"id":"T1","span":{"begin":262,"end":291},"obj":"Phenotype"},{"id":"T2","span":{"begin":293,"end":296},"obj":"Phenotype"},{"id":"T3","span":{"begin":729,"end":745},"obj":"Phenotype"},{"id":"T4","span":{"begin":971,"end":974},"obj":"Phenotype"},{"id":"T5","span":{"begin":1479,"end":1482},"obj":"Phenotype"}],"attributes":[{"id":"A1","pred":"hp_id","subj":"T1","obj":"HP:0007354"},{"id":"A2","pred":"hp_id","subj":"T2","obj":"HP:0007354"},{"id":"A3","pred":"hp_id","subj":"T3","obj":"HP:0025464"},{"id":"A4","pred":"hp_id","subj":"T4","obj":"HP:0007354"},{"id":"A5","pred":"hp_id","subj":"T5","obj":"HP:0007354"}],"namespaces":[{"prefix":"HP","uri":"http://purl.obolibrary.org/obo/HP_"}],"text":"Aggregation of the nucleic acid-binding protein TDP-43 occurs via distinct routes that are coordinated with stress granule formation.\nTAR DNA-binding protein 43 (TDP-43) is a nucleic acid-binding protein, and its aggregation represents the defining pathology in amyotrophic lateral sclerosis (ALS) and related proteinopathies. Recent studies implicate cytoplasmic stress granules (SGs) as hubs that may facilitate TDP-43 aggregation. Here, using cellular fractionation, biochemical analyses, and histological assays, we show that TDP-43 targeted to the cytoplasm has multiple fates. Whereas a TDP-43 subpopulation is indeed recruited to SGs, mature aggregated TDP-43, produced with aggregate-prone TDP-43 variants or exposure to oxidative stress, generates distinct TDP-43 inclusions that are surprisingly devoid of SGs. Consistent with this observation, we found that SG components are predominantly excluded from TDP-43 pathology in motor neurons from individuals with ALS. We generated de novo SGs by expressing the fragile X protein (FMRP) and found that rather than directly engaging TDP-43 aggregates, SGs can sequester the proteostasis factor histone deacetylase 6 (HDAC6) and thereby impede TDP-43 clearance from cells. These findings indicate that SGs form distinct cytoplasmic structures that can indirectly enhance TDP-43 aggregation. Therapeutic approaches that inhibit SG formation may therefore be effective at suppressing TDP-43-mediated toxicity in patients with ALS and related TDP-43 proteinopathies."}

    mondo_disease

    {"project":"mondo_disease","denotations":[{"id":"T1","span":{"begin":134,"end":137},"obj":"Disease"},{"id":"T2","span":{"begin":262,"end":291},"obj":"Disease"},{"id":"T3","span":{"begin":293,"end":296},"obj":"Disease"},{"id":"T4","span":{"begin":310,"end":325},"obj":"Disease"},{"id":"T5","span":{"begin":971,"end":974},"obj":"Disease"},{"id":"T6","span":{"begin":1479,"end":1482},"obj":"Disease"},{"id":"T7","span":{"begin":1502,"end":1517},"obj":"Disease"}],"attributes":[{"id":"A1","pred":"mondo_id","subj":"T1","obj":"http://purl.obolibrary.org/obo/MONDO_0010121"},{"id":"A2","pred":"mondo_id","subj":"T2","obj":"http://purl.obolibrary.org/obo/MONDO_0004976"},{"id":"A3","pred":"mondo_id","subj":"T3","obj":"http://purl.obolibrary.org/obo/MONDO_0004976"},{"id":"A4","pred":"mondo_id","subj":"T4","obj":"http://purl.obolibrary.org/obo/MONDO_0021179"},{"id":"A5","pred":"mondo_id","subj":"T5","obj":"http://purl.obolibrary.org/obo/MONDO_0004976"},{"id":"A6","pred":"mondo_id","subj":"T6","obj":"http://purl.obolibrary.org/obo/MONDO_0004976"},{"id":"A7","pred":"mondo_id","subj":"T7","obj":"http://purl.obolibrary.org/obo/MONDO_0021179"}],"text":"Aggregation of the nucleic acid-binding protein TDP-43 occurs via distinct routes that are coordinated with stress granule formation.\nTAR DNA-binding protein 43 (TDP-43) is a nucleic acid-binding protein, and its aggregation represents the defining pathology in amyotrophic lateral sclerosis (ALS) and related proteinopathies. Recent studies implicate cytoplasmic stress granules (SGs) as hubs that may facilitate TDP-43 aggregation. Here, using cellular fractionation, biochemical analyses, and histological assays, we show that TDP-43 targeted to the cytoplasm has multiple fates. Whereas a TDP-43 subpopulation is indeed recruited to SGs, mature aggregated TDP-43, produced with aggregate-prone TDP-43 variants or exposure to oxidative stress, generates distinct TDP-43 inclusions that are surprisingly devoid of SGs. Consistent with this observation, we found that SG components are predominantly excluded from TDP-43 pathology in motor neurons from individuals with ALS. We generated de novo SGs by expressing the fragile X protein (FMRP) and found that rather than directly engaging TDP-43 aggregates, SGs can sequester the proteostasis factor histone deacetylase 6 (HDAC6) and thereby impede TDP-43 clearance from cells. These findings indicate that SGs form distinct cytoplasmic structures that can indirectly enhance TDP-43 aggregation. Therapeutic approaches that inhibit SG formation may therefore be effective at suppressing TDP-43-mediated toxicity in patients with ALS and related TDP-43 proteinopathies."}

    Anatomy-MAT

    {"project":"Anatomy-MAT","denotations":[{"id":"T1","span":{"begin":274,"end":281},"obj":"Body_part"}],"attributes":[{"id":"A1","pred":"mat_id","subj":"T1","obj":"http://purl.obolibrary.org/obo/MAT_0000488"}],"text":"Aggregation of the nucleic acid-binding protein TDP-43 occurs via distinct routes that are coordinated with stress granule formation.\nTAR DNA-binding protein 43 (TDP-43) is a nucleic acid-binding protein, and its aggregation represents the defining pathology in amyotrophic lateral sclerosis (ALS) and related proteinopathies. Recent studies implicate cytoplasmic stress granules (SGs) as hubs that may facilitate TDP-43 aggregation. Here, using cellular fractionation, biochemical analyses, and histological assays, we show that TDP-43 targeted to the cytoplasm has multiple fates. Whereas a TDP-43 subpopulation is indeed recruited to SGs, mature aggregated TDP-43, produced with aggregate-prone TDP-43 variants or exposure to oxidative stress, generates distinct TDP-43 inclusions that are surprisingly devoid of SGs. Consistent with this observation, we found that SG components are predominantly excluded from TDP-43 pathology in motor neurons from individuals with ALS. We generated de novo SGs by expressing the fragile X protein (FMRP) and found that rather than directly engaging TDP-43 aggregates, SGs can sequester the proteostasis factor histone deacetylase 6 (HDAC6) and thereby impede TDP-43 clearance from cells. These findings indicate that SGs form distinct cytoplasmic structures that can indirectly enhance TDP-43 aggregation. Therapeutic approaches that inhibit SG formation may therefore be effective at suppressing TDP-43-mediated toxicity in patients with ALS and related TDP-43 proteinopathies."}

    Anatomy-UBERON

    {"project":"Anatomy-UBERON","denotations":[{"id":"T1","span":{"begin":352,"end":363},"obj":"Body_part"},{"id":"T2","span":{"begin":553,"end":562},"obj":"Body_part"},{"id":"T3","span":{"begin":935,"end":948},"obj":"Body_part"},{"id":"T4","span":{"begin":1275,"end":1286},"obj":"Body_part"}],"attributes":[{"id":"A1","pred":"uberon_id","subj":"T1","obj":"http://purl.obolibrary.org/obo/GO_0005737"},{"id":"A2","pred":"uberon_id","subj":"T2","obj":"http://purl.obolibrary.org/obo/GO_0005737"},{"id":"A3","pred":"uberon_id","subj":"T3","obj":"http://purl.obolibrary.org/obo/CL_0000100"},{"id":"A4","pred":"uberon_id","subj":"T4","obj":"http://purl.obolibrary.org/obo/GO_0005737"}],"text":"Aggregation of the nucleic acid-binding protein TDP-43 occurs via distinct routes that are coordinated with stress granule formation.\nTAR DNA-binding protein 43 (TDP-43) is a nucleic acid-binding protein, and its aggregation represents the defining pathology in amyotrophic lateral sclerosis (ALS) and related proteinopathies. Recent studies implicate cytoplasmic stress granules (SGs) as hubs that may facilitate TDP-43 aggregation. Here, using cellular fractionation, biochemical analyses, and histological assays, we show that TDP-43 targeted to the cytoplasm has multiple fates. Whereas a TDP-43 subpopulation is indeed recruited to SGs, mature aggregated TDP-43, produced with aggregate-prone TDP-43 variants or exposure to oxidative stress, generates distinct TDP-43 inclusions that are surprisingly devoid of SGs. Consistent with this observation, we found that SG components are predominantly excluded from TDP-43 pathology in motor neurons from individuals with ALS. We generated de novo SGs by expressing the fragile X protein (FMRP) and found that rather than directly engaging TDP-43 aggregates, SGs can sequester the proteostasis factor histone deacetylase 6 (HDAC6) and thereby impede TDP-43 clearance from cells. These findings indicate that SGs form distinct cytoplasmic structures that can indirectly enhance TDP-43 aggregation. Therapeutic approaches that inhibit SG formation may therefore be effective at suppressing TDP-43-mediated toxicity in patients with ALS and related TDP-43 proteinopathies."}