In the yeast two-hybrid library screening, the heart-specific FHL2 protein was found to interact with hCDC47. In vitro interaction study between FHL2 protein and hCDC47 was demonstrated. From the results of domain studies by the yeast two-hybrid assay, the second and third LIM domains in conjunction
Interaction of the heart-specific LIM domain protein, FHL2, with DNA-binding nuclear protein, hNP220
✍ Scribed by Enders Kai On Ng; Kwok Keung Chan; Chi Hang Wong; Stephen Kwok Wing Tsui; Sai Ming Ngai; Simon Ming Yuen Lee; Masayo Kotaka; Cheuk Yu Lee; Mary Miu Yee Waye; Kwok Pui Fung
- Publisher
- John Wiley and Sons
- Year
- 2002
- Tongue
- English
- Weight
- 223 KB
- Volume
- 84
- Category
- Article
- ISSN
- 0730-2312
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✦ Synopsis
Abstract
Using a yeast two‐hybrid library screen, we have identified that the heart specific FHL2 protein, four‐and‐a‐half LIM protein 2, interacted with human DNA‐binding nuclear protein, hNP220. Domain studies by the yeast two‐hybrid interaction assay revealed that the second LIM domain together with the third and the fourth LIM domains of FHL2 were responsible to the binding with hNP220. Using green fluorescent protein (GFP)‐FHL2 and blue fluorescent protein (BFP)‐hNP220 fusion proteins co‐expressed in the same cell, we demonstrated a direct interaction between FHL2 and hNP220 in individual nucleus by two‐fusion Fluorescence Resonance Energy Transfer (FRET) assay. Besides, Western blot analysis using affinity‐purified anti‐FHL2 antipeptide antibodies confirmed a 32‐kDa protein of FHL2 in heart only. Virtually no expression of FHL2 protein was detected in brain, liver, lung, kidney, testis, skeletal muscle, and spleen. Moreover, the expression of FHL2 protein was also detectable in the human diseased heart tissues. Our results imply that FHL2 protein can shuttle between cytoplasm and nucleus and may act as a molecular adapter to form a multicomplex with hNP220 in the nucleus, thus we speculate that FHL2 may be particularly important for heart muscle differentiation and the maintenance of the heart phenotype. J. Cell. Biochem. 84: 556–566, 2002. © 2001 Wiley‐Liss, Inc.
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