NUMB adaptoriproteiini osallistuu luumassan ylläpitoon , antituumorivaikutuksia .

https://www.ncbi.nlm.nih.gov/pubmed/30455992

Bone Res. 2018 Nov 10;6:32. doi: 10.1038/s41413-018-0030-y. eCollection 2018.

NUMB maintains bone mass by promoting degradation of PTEN and GLI1 via ubiquitination in osteoblasts.

Ye L¹, Lou F¹, Yu F¹, Zhang D¹, Wang C¹, Wu F¹, Li X¹, Ping Y¹, Yang X¹, Yang J¹, Chen D¹, Gao B¹, Huang D¹, Liu P².Abstract

Adaptoriprotieini NUMB osallistuu asymmteriseen solunjakautumiseen ja solukohtalon määräämiseen ja se on  tunnistettu NOTCH- antagonistina.

Aiemmissa tutkimuksissa on osoitautunut, että Notch-aktivaatio osteoblasteissa  vaikuttaa korkeaa luumassaa.

 Tässä tutkimuksessa kuitenkin hiiren osteopeninen fenotyyppi  havaittiin  9-viikkoisessa hiiressä  käyttämällä osteoblastipesifistä Col1alfa-2.3-Cre , joka  teki ablaation sekä Numb:iin  että  sen homolgiin Numbl. Trabekulaarinen luumassa väheni dramaattisesti kun taas kortikaalinen luumassa ei vaikuttunut. Tässä ei NOTCH signaali  aktivoitunut, kun taas PTEN  (PI3kinasien  defosforyloija) oli koholla  vaimentaen PKB (Akt) . 

Ubikitinaatiomenetelmällä  selvisi, että NUMB saattaa fysiologisesti edistää PTEN-ubikitinaatiota, jos läsnä  on erästä neuronin esiasteessa kehityksellisti alassäätynyttä  proteiinia.

 Lisäksi Numb/Numbl vaje  aktivoi Hedgehog tien GLII- kautta.  Tämän prosessin  vaikuttavan  NFKB tien suhdetta  ostoprotegeriiniin, joka  lisää osteoklastien  erilaistumista ja luun resorptiota . Johtopäätös täten  on, että  NUMB ja NUMBL  voivat  vaikuttaa luun homeostaassiin.

• The adaptor protein NUMB is involved in asymmetric division and cell fate determination and recognized as an antagonist of Notch. Previous studies have proved that Notch activation in osteoblasts contributes to a high bone mass. In this study,  however, an osteopenic phenotype was found in 9-week-old mice using osteoblastic specific Col1a1-2.3-Cre to ablate both Numb and its homologue Numbl . The trabecular bone mass decreased dramatically while the cortical bone mass was unaffected. Here, the Notch signal was not activated, while the tensin homologue deleted on human chromosome 10 (PTEN), which dephosphorylates phosphatidylinositide 3-kinases, was elevated, attenuating protein kinase B (Akt). The ubiquitination assay revealed that NUMB may physiologically promote PTEN ubiquitination in the presence of neural precursor cell-expressed developmentally downregulated protein 4-1. In addition, the deficiency of Numb/Numbl also activated the Hedgehog pathway through GLI1. This process was found to improve the ratio of the receptor activator of nuclear factor-kB ligand to osteoprotegerin, which enhanced the differentiation of osteoclasts and bone resorption . In conclusion, this study provides an insight into  new functons of   NUMB and NUMBL on bone homeostasis.

PMID:

30455992

PMCID:

PMC6226489

DOI:

10.1038/s41413-018-0030-y

Free PMC Article

Gene NUMB (14q24.2.-q24.3)  

https://www.ncbi.nlm.nih.gov/gene/8650

S171; C14orf41; c14_5527

Summary

The protein encoded by this gene plays a role in the determination of cell fates during development. The encoded protein, whose degradation is induced in a proteasome-dependent manner by MDM2, is a membrane-bound protein that has been shown to associate with EPS15, LNX1, and NOTCH1. Alternative splicing results in multiple transcript variants. [provided by RefSeq, Feb 2016]

Expression

Ubiquitous expression in lung (RPKM 25.7), gall bladder (RPKM 21.4) and 25 other tissues See more

Preferred Names

protein numb homolog

Names

h-Numb

numb homolog

Conserved Domains (2) summary

cd01268
Location:23 → 168

PTB_Numb; Numb Phosphotyrosine-binding (PTB) domain

pfam06311
Location:258 → 338

NumbF; NUM

 

protein numb homolog isoform 1 [Homo sapiens]

NCBI Reference Sequence: NP_001005743.1

Identical Proteins FASTA Graphics

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LOCUS       NP_001005743             651 aa            linear   PRI 11-NOV-2018
DEFINITION  protein numb homolog isoform 1 [Homo sapiens].
ACCESSION   NP_001005743
VERSION     NP_001005743.1
DBSOURCE    REFSEQ: accession NM_001005743.1
KEYWORDS    RefSeq.
SOURCE      Homo sapiens (human)
  ORGANISM  Homo sapiens
            Eukaryota; Metazoa; Chordata; Craniata; Vertebrata; Euteleostomi;
            Mammalia; Eutheria; Euarchontoglires; Primates; Haplorrhini;
            Catarrhini; Hominidae; Homo.
REFERENCE   1  (residues 1 to 651)
  AUTHORS   Zhang C, Kang Y, Ma R, Chen F, Chen F and Dong X.
  TITLE     Expression of Numb and Gli1 in malignant pleural mesothelioma and
            their clinical significance
  JOURNAL   J Cancer Res Ther 14 (5), 970-976 (2018)
   PUBMED   30197333
  REMARK    GeneRIF: The results provide new evidence of Numb and Gli1 on the
            clinical characteristics of Malignant pleural mesothelioma, which
            may be helpful in clinical diagnosis and targeted therapy. Further
            research with larger sample size is needed
REFERENCE   2  (residues 1 to 651)
  AUTHORS   Schuring AN, Dahlhues B, Korte A, Kiesel L, Titze U, Heitkotter B,
            Ruckert C and Gotte M.
  TITLE     The endometrial stem cell markers notch-1 and numb are associated
            with endometriosis
  JOURNAL   Reprod. Biomed. Online 36 (3), 294-301 (2018)
   PUBMED   29398419
  REMARK    GeneRIF: High NUMB expression is associated with endometriosis.
REFERENCE   3  (residues 1 to 651)
  AUTHORS   Colaluca IN, Basile A, Freiburger L, D'Uva V, Disalvatore D, Vecchi
            M, Confalonieri S, Tosoni D, Cecatiello V, Malabarba MG, Yang CJ,
            Kainosho M, Sattler M, Mapelli M, Pece S and Di Fiore PP.
  TITLE     A Numb-Mdm2 fuzzy complex reveals an isoform-specific involvement
            of Numb in breast cancer
  JOURNAL   J. Cell Biol. 217 (2), 745-762 (2018)
   PUBMED   29269425
REFERENCE   4  (residues 1 to 651)
  AUTHORS   Guo Y, Zhang K, Cheng C, Ji Z, Wang X, Wang M, Chu M, Tang DG, Zhu
            HH and Gao WQ.
  TITLE     Numb(-/low) Enriches a Castration-Resistant Prostate Cancer Cell
            Subpopulation Associated with Enhanced Notch and Hedgehog Signaling
  JOURNAL   Clin. Cancer Res. 23 (21), 6744-6756 (2017)
   PUBMED   28751447
  REMARK    GeneRIF: Numb(-/low) prostate cancer cells were smaller and
            quiescent, preferentially expressed Notch and Hedgehog downstream
            and stem-cell-associated genes, and associated with a greater
            resistance to androgen-deprivation therapy
REFERENCE   5  (residues 1 to 651)
  AUTHORS   Bocci F, Jolly MK, Tripathi SC, Aguilar M, Hanash SM, Levine H and
            Onuchic JN.
  TITLE     Numb prevents a complete epithelial-mesenchymal transition by
            modulating Notch signalling
  JOURNAL   J R Soc Interface 14 (136) (2017)
   PUBMED   29187638
  REMARK    GeneRIF: Numb is associated with modulation of Notch-driven
            epithelial-mesenchymal transition.
REFERENCE   6  (residues 1 to 651)
  AUTHORS   Dho SE, Jacob S, Wolting CD, French MB, Rohrschneider LR and
            McGlade CJ.
  TITLE     The mammalian numb phosphotyrosine-binding domain. Characterization
            of binding specificity and identification of a novel PDZ
            domain-containing numb binding protein, LNX
  JOURNAL   J. Biol. Chem. 273 (15), 9179-9187 (1998)
   PUBMED   9535908
REFERENCE   7  (residues 1 to 651)
  AUTHORS   Salcini AE, Confalonieri S, Doria M, Santolini E, Tassi E,
            Minenkova O, Cesareni G, Pelicci PG and Di Fiore PP.
  TITLE     Binding specificity and in vivo targets of the EH domain, a novel
            protein-protein interaction module
  JOURNAL   Genes Dev. 11 (17), 2239-2249 (1997)
   PUBMED   9303539
REFERENCE   8  (residues 1 to 651)
  AUTHORS   Zhong W, Feder JN, Jiang MM, Jan LY and Jan YN.
  TITLE     Asymmetric localization of a mammalian numb homolog during mouse
            cortical neurogenesis
  JOURNAL   Neuron 17 (1), 43-53 (1996)
   PUBMED   8755477
REFERENCE   9  (residues 1 to 651)
  AUTHORS   Wong WT, Schumacher C, Salcini AE, Romano A, Castagnino P, Pelicci
            PG and Di Fiore PP.
  TITLE     A protein-binding domain, EH, identified in the receptor tyrosine
            kinase substrate Eps15 and conserved in evolution
  JOURNAL   Proc. Natl. Acad. Sci. U.S.A. 92 (21), 9530-9534 (1995)
   PUBMED   7568168
REFERENCE   10 (residues 1 to 651)
  AUTHORS   Sherrington R, Rogaev EI, Liang Y, Rogaeva EA, Levesque G, Ikeda M,
            Chi H, Lin C, Li G, Holman K, Tsuda T, Mar L, Foncin JF, Bruni AC,
            Montesi MP, Sorbi S, Rainero I, Pinessi L, Nee L, Chumakov I,
            Pollen D, Brookes A, Sanseau P, Polinsky RJ, Wasco W, Da Silva HA,
            Haines JL, Perkicak-Vance MA, Tanzi RE, Roses AD, Fraser PE,
            Rommens JM and St George-Hyslop PH.
  TITLE     Cloning of a gene bearing missense mutations in early-onset
            familial Alzheimer's disease
  JOURNAL   Nature 375 (6534), 754-760 (1995)
   PUBMED   7596406
COMMENT     REVIEWED REFSEQ: This record has been curated by NCBI staff. The
            reference sequence was derived from BC068476.1, AF171938.1 and
            AA872908.1.
            This sequence is a reference standard in the RefSeqGene project.
            
            Summary: The protein encoded by this gene plays a role in the
            determination of cell fates during development. The encoded
            protein, whose degradation is induced in a proteasome-dependent
            manner by MDM2, is a membrane-bound protein that has been shown to
            associate with EPS15, LNX1, and NOTCH1. Alternative splicing
            results in multiple transcript variants. [provided by RefSeq, Feb
            2016].
            
            Transcript Variant: This variant (1) represents the longest
            transcript and encodes the longest isoform (1).
            
            Publication Note:  This RefSeq record includes a subset of the
            publications that are available for this gene. Please see the Gene
            record to access additional publications.
            
            ##Evidence-Data-START##
            Transcript exon combination :: AF171938.1 [ECO:0000332]
            RNAseq introns              :: mixed/partial sample support
                                           SAMEA1965299, SAMEA1966682
                                           [ECO:0000350]
            ##Evidence-Data-END##
FEATURES             Location/Qualifiers
     source          1..651
                     /organism="Homo sapiens"
                     /db_xref="taxon:9606"
                     /chromosome="14"
                     /map="14q24.2-q24.3"
     Protein         1..651
                     /product="protein numb homolog isoform 1"
                     /note="protein numb homolog; h-Numb"
                     /calculated_mol_wt=70673
     Region          23..168
                     /region_name="PTB_Numb"
                     /note="Numb Phosphotyrosine-binding (PTB) domain; cd01268"
                     /db_xref="CDD:241298"
     Site            order(42,125,145)
                     /site_type="other"
                     /note="putative phosphoinositide binding site [chemical
                     binding]"
                     /db_xref="CDD:241298"
     Site            order(55,116..119,155,159,162,166)
                     /site_type="other"
                     /note="peptide binding site [polypeptide binding]"
                     /db_xref="CDD:241298"
     Site            194
                     /site_type="other"
                     /experiment="experimental evidence, no additional details
                     recorded"
                     /note="Phosphoserine. {ECO:0000244|PubMed:23186163};
                     propagated from UniProtKB/Swiss-Prot (P49757.2)"
     Site            243
                     /site_type="other"
                     /experiment="experimental evidence, no additional details
                     recorded"
                     /note="Phosphothreonine. {ECO:0000250|UniProtKB:Q9QZS3};
                     propagated from UniProtKB/Swiss-Prot (P49757.2)"
     Site            244
                     /site_type="other"
                     /experiment="experimental evidence, no additional details
                     recorded"
                     /note="Phosphoserine. {ECO:0000244|PubMed:18669648};
                     propagated from UniProtKB/Swiss-Prot (P49757.2)"
     Region          258..338
                     /region_name="NumbF"
                     /note="NUMB domain; pfam06311"
                     /db_xref="CDD:283874"
     Site            276
                     /site_type="other"
                     /experiment="experimental evidence, no additional details
                     recorded"
                     /note="Phosphoserine, by CaMK1.
                     {ECO:0000250|UniProtKB:Q2LC84}; propagated from
                     UniProtKB/Swiss-Prot (P49757.2)"
     Site            295
                     /site_type="other"
                     /experiment="experimental evidence, no additional details
                     recorded"
                     /note="Phosphoserine, by CaMK1.
                     {ECO:0000250|UniProtKB:Q2LC84}; propagated from
                     UniProtKB/Swiss-Prot (P49757.2)"
     Site            425
                     /site_type="other"
                     /experiment="experimental evidence, no additional details
                     recorded"
                     /note="Phosphoserine. {ECO:0000244|PubMed:23186163};
                     propagated from UniProtKB/Swiss-Prot (P49757.2)"
     Site            436
                     /site_type="other"
                     /experiment="experimental evidence, no additional details
                     recorded"
                     /note="Phosphothreonine. {ECO:0000244|PubMed:23186163};
                     propagated from UniProtKB/Swiss-Prot (P49757.2)"
     Site            438
                     /site_type="other"
                     /experiment="experimental evidence, no additional details
                     recorded"
                     /note="Phosphoserine. {ECO:0000244|PubMed:23186163,
                     ECO:0000244|PubMed:24275569}; propagated from
                     UniProtKB/Swiss-Prot (P49757.2)"
     Site            634
                     /site_type="other"
                     /experiment="experimental evidence, no additional details
                     recorded"
                     /note="Phosphoserine. {ECO:0000244|PubMed:16964243,
                     ECO:0000244|PubMed:23186163}; propagated from
                     UniProtKB/Swiss-Prot (P49757.2)"
     CDS             1..651
                     /gene="NUMB"
                     /gene_synonym="C14orf41; c14_5527; S171"
                     /coded_by="NM_001005743.1:321..2276"
                     /note="isoform 1 is encoded by transcript variant 1"
                     /db_xref="CCDS:CCDS32116.1"
                     /db_xref="GeneID:8650"
                     /db_xref="HGNC:HGNC:8060"
                     /db_xref="MIM:603728"
ORIGIN      
        1 mnklrqsfrr kkdvyvpeas rphqwqtdee gvrtgkcsfp vkylghvevd esrgmhiced
       61 avkrlkaerk ffkgffgktg kkavkavlwv sadglrvvde ktkdlivdqt iekvsfcapd
      121 rnfdrafsyi crdgttrrwi chcfmavkdt gerlshavgc afaaclerkq krekecgvta
      181 tfdasrttft regsfrvtta teqaereeim kqmqdakkae tdkivvgssv apgntapsps
      241 sptsptsdat tslemnnpha iprrhapieq larqgsfrgf palsqkmspf krqlslrine
      301 lpstmqrktd fpiknavpev egeaesissl csqitnafst pedpfssapm tkpvtvvapq
      361 sptfqangtd safhvlakpa htalapvamp vretnpwaha pdaankeiaa tcsgtewgqs
      421 sgaaspglfq aghrrtpsea drwleevsks vraqqpqasa aplqpvlqpp pptaisqpas
      481 pfqgnaflts qpvpvgvvpa lqpafvpaqs ypvangmpyp apnvpvvgit psqmvanvfg
      541 taghpqaahp hqspslvrqq tfphyeassa ttspffkppa qhlngsaafn gvddgrlasa
      601 drhtevptgt cpvdpfeaqw aalenkskqr tnpsptnpfs sdlqktfeie l
//

Related articles in PubMed

1. Numb prevents a complete epithelial-mesenchymal transition (EMT) by modulating Notch signalling. Bocci F, et al. J R Soc Interface, 2017 Nov. PMID 29187638, Free PMC Article
2. Numb^-/low Enriches a Castration-Resistant Prostate Cancer Cell Subpopulation Associated with Enhanced Notch and Hedgehog Signaling. Guo Y, et al. Clin Cancer Res, 2017 Nov 1. PMID 28751447
3. Numb positively regulates autophagic flux via regulating lysosomal function. Sun H, et al. Biochem Biophys Res Commun, 2017 Sep 23. PMID 28720501
4. Numb had anti-tumor effects in prostatic cancer. Sun J, et al. Biomed Pharmacother, 2017 Aug. PMID 28531799
5. Pre-clinical validation of a selective anti-cancer stem cell therapy for Numb-deficient human breast cancers. Tosoni D, et al. EMBO Mol Med, 2017 May. PMID 28298340, Free PMC Article

See all (133) citations in PubMed

See citations in PubMed for homologs of this gene provided by HomoloGene

GeneRIFs: Gene References Into FunctionsWhat's a GeneRIF?

1. High NUMB expression is associated with endometriosis.
2. The results provide new evidence of Numb and Gli1 on the clinical characteristics of Malignant pleural mesothelioma, which may be helpful in clinical diagnosis and targeted therapy. Further research with larger sample size is needed
3. Numb is associated with modulation of Notch-driven epithelial-mesenchymal transition.
4. Numb(-/low) prostate cancer cells were smaller and quiescent, preferentially expressed Notch and Hedgehog downstream and stem-cell-associated genes, and associated with a greater resistance to androgen-deprivation therapy
5. MAP17 overexpression activates Notch pathway by sequestering NUMB. High levels of MAP17 correlated with tumorsphere formation and Notch and Stem gene transcription. Its direct modification causes direct alteration of tumorsphere number and Notch and Stem pathway transcription
6. NUMB has a role in negatively regulating the epithelial-mesenchymal transition of triple-negative breast cancer by antagonizing Notch signaling
7. In the present study, we identified that the adaptor protein Numb, which is demonstrated to be a novel binding partner of NEDD4-1, plays important roles in controlling PTEN ubiquitination through regulating NEDD4-1 activity and the association between PTEN and NEDD4-1.
8. Numb expression is not associated with favorable prognosis in small cell lung cancer.
9. Data suggest that over-expression of NUMB has anti-cancer effects to prostatic cancer cells; these studies included experiments both in vitro and in vivo (xenograft experiments in nude mice).
10. Using patient-derived xenografts, the study shows that expansion of the cancer stem cells pool, due to altered self-renewing divisions, is also a feature of Numb-deficient human breast cancers .

Submit: New GeneRIF Correction See all GeneRIFs (74)