The Tumor Suppressor Protein Fhit. A Novel Interaction with Tubulin

Overview

Journal J Biol Chem

Specialty Biochemistry

Date 1999 Aug 14

PMID 10446217

Citations 17

Authors

A R Chaudhuri

I A Khan

V Prasad

A K Robinson

R F Luduena

L D Barnes

Affiliations

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Abstract

FHIT (fragile histidine triad) is a candidate human tumor suppressor gene located at chromosome 3p14.2, a location that encompasses the FRA3B chromosomal fragile site. Aberrant transcripts have been detected in a variety of primary tumors, and homozygous deletions in the FHIT locus have been detected in different tumor cell lines. The gene product Fhit in vitro possesses the ability to hydrolyze diadenosine 5',5"'-P(1),P(3)-triphosphate (Ap(3)A). The mechanism of action of Fhit as a tumor suppressor is unknown. Because the tubulin-microtubule system plays an important role in cell division and cell proliferation, we investigated the interaction between wild-type Fhit or mutant Fhit (H96N) and tubulin in vitro. The mutant form of Fhit (H96N) lacks Ap(3)A hydrolase activity but retains tumor suppressor activity. We found that both wild-type and mutated forms of Fhit bind to tubulin strongly and specifically with K(d) values of 1.4 and 2.1 microM, respectively. Neither wild-type nor mutant Fhit cause nucleation or formation of microtubules, but in the presence of microtubule-associated proteins, both wild-type and mutant Fhit promote assembly to a greater extent than do microtubule-associated proteins alone, and the microtubules formed appear normal by electron microscopy. Our results suggest the possibility that Fhit may exert its tumor suppressor activity by interacting with microtubules and also indicate that the interaction between Fhit and tubulin is not related to the Ap(3)A hydrolase activity of Fhit.

Citing Articles

Chemical Proteomics of the Tumor Suppressor Fhit Covalently Bound to the Cofactor ApA Elucidates Its Inhibitory Action on Translation.

Herzog D, Jansen J, Missun M, Diederichs K, Stengel F, Marx A J Am Chem Soc. 2022; 144(19):8613-8623.

PMID: 35522782 PMC: 9121386. DOI: 10.1021/jacs.2c00815.

Upregulation of FHIT gene expression in endometrial carcinoma by RNA activation.

Zhu Q, Wu X, Huang Y, Tang M, Wu L Int J Clin Exp Pathol. 2020; 13(6):1372-1380.

PMID: 32661472 PMC: 7344018.

Fhit-Fdxr interaction in the mitochondria: modulation of reactive oxygen species generation and apoptosis in cancer cells.

Druck T, Cheung D, Park D, Trapasso F, Pichiorri F, Gaspari M Cell Death Dis. 2019; 10(3):147.

PMID: 30770797 PMC: 6377664. DOI: 10.1038/s41419-019-1414-7.

Fhit, a tumor suppressor protein, induces autophagy via 14-3-3τ in non-small cell lung cancer cells.

Lee T, Jeong E, Kim S, Kim H, Kim H, Kim C Oncotarget. 2017; 8(19):31923-31937.

PMID: 28404875 PMC: 5458259. DOI: 10.18632/oncotarget.16652.

Src family kinases and paclitaxel sensitivity.

Le X, Bast Jr R Cancer Biol Ther. 2011; 12(4):260-9.

PMID: 21646863 PMC: 3173729. DOI: 10.4161/cbt.12.4.16430.