Disruption of Bcr-Abl Coiled Coil Oligomerization by Design

Dixon, Andrew S.; Pendley, Scott S.; Bruno, Benjamin; Woessner, David W.; Shimpi, Adrian A.; Cheatham, Thomas E.; Lim, Carol S.

doi:10.1074/jbc.m111.264903

Cited by 27 publications

(109 citation statements)

References 54 publications

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“…3, 4 We have previously reported a modified version of this coiled-coil domain, CCmut2, which exhibits disruption of Bcr-Abl oligomeric complexes and results in decreased proliferation of CML cells and induction of apoptosis. 5 A major contributing factor to these enhanced capabilities is the destabilization of the CCmut2 homo-dimers, increasing the availability to interact with and inhibit Bcr-Abl. Here, we included an additional mutation (K39E) that could in turn further destabilize the mutant homo-dimer.…”

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confidence: 99%

Improved Coiled-Coil Design Enhances Interaction with Bcr-Abl and Induces Apoptosis

et al. 2011

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The oncoprotein Bcr-Abl drives aberrant downstream activity through trans-autophosphorylation of homo-oligomers in chronic myelogenous leukemia (CML).1,2 The formation of Bcr-Abl oligomers is achieved through the coiled-coil domain at the N-terminus of Bcr.3, 4 We have previously reported a modified version of this coiled-coil domain, CCmut2, which exhibits disruption of Bcr-Abl oligomeric complexes and results in decreased proliferation of CML cells and induction of apoptosis.5 A major contributing factor to these enhanced capabilities is the destabilization of the CCmut2 homo-dimers, increasing the availability to interact with and inhibit Bcr-Abl. Here, we included an additional mutation (K39E) that could in turn further destabilize the mutant homo-dimer. Incorporation of this modification into CCmut2 (C38A, S41R, L45D, E48R, Q60E) generated what we termed CCmut3, and resulted in further improvements in the binding properties with the wild-type coiled-coil domain representative of Bcr-Abl. A separate construct containing one revert mutation, CCmut4, did not demonstrate improved oligomeric properties and indicated the importance of the L45D mutation. CCmut3 demonstrated improved oligomerization via a two-hybrid assay as well as through colocalization studies, in addition to showing similar biologic activity as CCmut2. The improved binding between CCmut3 and the Bcr-Abl coiled-coil may be used to redirect Bcr-Abl to alternative subcellular locations with interesting therapeutic implications.

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confidence: 99%

Improved Coiled-Coil Design Enhances Interaction with Bcr-Abl and Induces Apoptosis

et al. 2011

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“…In oncogenic ALK-fusions oligomerization conferred by the fusion partner mimics the native oligomerization-dependent activation mechanism of receptor tyrosine kinases and engenders constitutive activation of ALK [25]. The use of rationally-designed peptide and peptidomimetic inhibitors is under investigation for the disruption of several coiled-coil interactions that are implicated in disease and clinically useful therapeutics have been developed using this approach [27,28,29]. The TD structures may enable the development of protein-protein interaction inhibitors targeting the trimerization interface of the EML4 TD, another possible avenue towards therapeutic intervention in EML4-ALK NSCLC and one that would be applicable to all variants.…”

Section: Discussionmentioning

confidence: 99%

Microtubule association of EML proteins and the EML4-ALK variant 3 oncoprotein require an N-terminal trimerization domain

Richards

O’Regan

Röth

et al. 2015

Biochemical Journal

103

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The structural co-ordinates reported for EML2 11-60 and EML4 6-64 I38M appear in the PDB under codes 4CGB and 4CGC respectively. Page heading: EML trimerization domain drives MT-bindingKeywords: EML1, EML2, EML4-ALK, crystal structure, coiled-coil, microtubule 2 SUMMARY STATEMENTWe present crystal structures of a trimeric coiled-coil domain found in EML proteins. This trimerization domain mediates self-association and interactions between a subset of EML proteins. Microtubule-association of EML proteins requires the trimerization domain and an adjacent basic region. ABSTRACTProteins of the echinoderm microtubule associated protein-like (EML) family contribute to formation of the mitotic spindle and interphase microtubule (MT) network. EML1-4 consist of WD40 repeats and an N-terminal region containing a putative coiled-coil. Recurrent gene rearrangements in nonsmall cell lung cancer (NSCLC) fuse EML4 to anaplastic lymphoma kinase (ALK) causing expression of several oncogenic fusion variants. The fusions have constitutive ALK activity due to self-association through the EML4 coiled-coil. We have determined crystal structures of the coiledcoils from EML2 and EML4, which describe the structural basis of both EML self-association and oncogenic EML4-ALK activation. The structures reveal a trimeric oligomerization state directed by a conserved pattern of hydrophobic residues and salt bridges. We show that the trimerization domain (TD) of EML1 is necessary and sufficient for self-association. The TD is also essential for MT binding, however this property requires an adjacent basic region. These observations prompted us to investigate MT association of EML4-ALK and EML1-ABL1 fusions in which variable portions of the EML component are present. Uniquely, EML4-ALK variant 3, which includes the TD and basic region of EML4 but none of the WD40 repeats, was localized to MTs, both when expressed recombinantly and in a patient-derived NSCLC cell line (H2228). This raises the question of whether the mislocalization of ALK activity to MTs might influence downstream signalling and malignant properties of cells. Furthermore, the structure of EML4 TD may enable the development of protein-protein interaction inhibitors targeting the trimerization interface, providing a possible avenue towards therapeutic intervention in EML4-ALK NSCLC.

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“…Previous studies have demonstrated that all of them are validated for use (Aguilera et al, 2011;Averous et al, 2012;Della Pietra et al, 2015;Dixon et al, 2011;Gong et al, 2015;Kim et al, 2011;Li et al, 2012;Murphy et al, 2011;Nissar et al, 2012;Rao et al, 2014;Sarkar and Zohn, 2012;Takeda et al, 2014;Tan et al, 2011;Taniguchi et al, 2011;Wu et al, 2010;Zhang et al, 2011).…”

Section: Antibodiesmentioning

confidence: 99%

HMGB2 regulates satellite-cell-mediated skeletal muscle regeneration through IGF2BP2

Zhou

Huang

et al. 2016

Journal of Cell Science

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Although the mechanism underlying modulation of transcription factors in myogenesis has been well elucidated, the function of the transcription cofactors involved in this process remains poorly understood. Here, we identified HMGB2 as an essential nuclear transcriptional co-regulator in myogenesis. HMGB2 was highly expressed in undifferentiated myoblasts and regenerating muscle. Knockdown of HMGB2 inhibited myoblast proliferation and stimulated its differentiation. HMGB2 depletion downregulated Myf5 and cyclin A2 at the protein but not mRNA level. In contrast, overexpression of HMGB2 promoted Myf5 and cyclin A2 protein upregulation. Furthermore, we found that the RNA-binding protein IGF2BP2 is a downstream target of HMGB2, as previously shown for HMGA2. IGF2BP2 binds to mRNAs of Myf5 or cyclin A2, resulting in translation enhancement or mRNA stabilization, respectively. Notably, overexpression of IGF2BP2 could partially rescue protein levels of Myf5 and cyclin A2, in response to HMGB2 decrease. Moreover, depletion of HMGB2 in vivo severely attenuated muscle repair; this was due to a decrease in satellite cells. Taken together, these results highlight the previously undiscovered and crucial role of the HMGB2-IGF2BP2 axis in myogenesis and muscle regeneration.

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Disruption of Bcr-Abl Coiled Coil Oligomerization by Design

Cited by 27 publications

References 54 publications

Improved Coiled-Coil Design Enhances Interaction with Bcr-Abl and Induces Apoptosis

Improved Coiled-Coil Design Enhances Interaction with Bcr-Abl and Induces Apoptosis

Microtubule association of EML proteins and the EML4-ALK variant 3 oncoprotein require an N-terminal trimerization domain

HMGB2 regulates satellite-cell-mediated skeletal muscle regeneration through IGF2BP2

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