Literature DB >> 31407015

Promiscuous Dimerization Between the Caenorhabditis elegans IF Proteins and a Hypothesis to Explain How Multiple IFs Persist Over Evolutionary Time.

Anton Karabinos1, Jürgen Schünemann2, David A D Parry3.   

Abstract

Our previous calculations of ionic interactions indicated that the Caenorhabditis elegans intermediate filament (IF) IFA proteins, in addition to IFA/IFB-1 heterodimers, may also form homodimers. In order to prove the significance of these calculations, we analysed the dimerization potential of the IFA chains in blot overlays. Unexpectedly, we found here that the dimerization of the IFA-1 protein was of both homotypic and heterotypic nature, and involved all proteins immobilized on the membrane (IFA-1, IFA-2, IFA-4, IFB-1, IFB-2, IFC-1, IFC-2, IFD-1, IFD-2 and IFP-1). A similar interaction profile, though less complex, was observed for two biotinylated proteins (IFA-2 and IFA-4). These and previous results indicate that the IFA proteins are able to form many different heteropolymeric and homopolymeric complexes in the C. elegans tissue, but that only those triggered by the IFA-specific IFB-1 protein result in mature IFs. Moreover, the calculations of the possible ionic interactions between the individual rod sequences as well as their various deletion variants indicated a special role in this process for the middle part of the C. elegans IF coil 1B segment that is deleted in all vertebrate cytoplasmic IFs. We hypothesized here, therefore, that the striking promiscuity of the C. elegans IFs originally involved a nuclear lamin which, due to a two-heptad-long rod deletion, prevented formation of a functional lamin/cIF dimer. This, in concert with an efficient dimerization and a strict tissue-specific co-expression, may allow expansion and maintenance of the multiple Caenorhabditis IFs. A possible implication for evolution of chordate IFs proteins is also discussed.

Entities:  

Keywords:  C. elegans; Dimers; Evolution; Intermediate filament; Lamin; Nematode

Mesh:

Substances:

Year:  2019        PMID: 31407015     DOI: 10.1007/s00239-019-09904-5

Source DB:  PubMed          Journal:  J Mol Evol        ISSN: 0022-2844            Impact factor:   2.395


  51 in total

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3.  Functional genomic analysis of C. elegans chromosome I by systematic RNA interference.

Authors:  A G Fraser; R S Kamath; P Zipperlen; M Martinez-Campos; M Sohrmann; J Ahringer
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Review 4.  Human keratin diseases: the increasing spectrum of disease and subtlety of the phenotype-genotype correlation.

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Journal:  Br J Dermatol       Date:  1999-05       Impact factor: 9.302

5.  Characterization of the Hydra lamin and its gene: A molecular phylogeny of metazoan lamins.

Authors:  A Erber; D Riemer; H Hofemeister; M Bovenschulte; R Stick; G Panopoulou; H Lehrach; K Weber
Journal:  J Mol Evol       Date:  1999-08       Impact factor: 2.395

6.  Human and Xenopus cingulin share a modular organization of the coiled-coil rod domain: predictions for intra- and intermolecular assembly.

Authors:  S Citi; F D'Atri; D A Parry
Journal:  J Struct Biol       Date:  2000-08       Impact factor: 2.867

7.  Essential roles for four cytoplasmic intermediate filament proteins in Caenorhabditis elegans development.

Authors:  A Karabinos; H Schmidt; J Harborth; R Schnabel; K Weber
Journal:  Proc Natl Acad Sci U S A       Date:  2001-06-26       Impact factor: 11.205

8.  Essential roles for Caenorhabditis elegans lamin gene in nuclear organization, cell cycle progression, and spatial organization of nuclear pore complexes.

Authors:  J Liu; T Rolef Ben-Shahar; D Riemer; M Treinin; P Spann; K Weber; A Fire; Y Gruenbaum
Journal:  Mol Biol Cell       Date:  2000-11       Impact factor: 4.138

9.  Targeted deletion of keratins 18 and 19 leads to trophoblast fragility and early embryonic lethality.

Authors:  M Hesse; T Franz; Y Tamai; M M Taketo; T M Magin
Journal:  EMBO J       Date:  2000-10-02       Impact factor: 11.598

10.  Myotactin, a novel hypodermal protein involved in muscle-cell adhesion in Caenorhabditis elegans.

Authors:  M C Hresko; L A Schriefer; P Shrimankar; R H Waterston
Journal:  J Cell Biol       Date:  1999-08-09       Impact factor: 10.539

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