Evidence for Interaction Between Human PRUNE and Nm23-H1 NDPKinase

Overview

Journal Oncogene

Specialties Molecular Biology
Oncology

Date 1999 Dec 22

PMID 10602478

Citations 38

Authors

A Reymond

S Volorio

G Merla

O Zuffardi

A Bulfone

A Ballabio

M Zollo

Affiliations

Soon will be listed here.

Abstract

We have isolated a human and murine homologue of the Drosophila prune gene through dbEST searches. The gene is ubiquitously expressed in human adult tissues, while in mouse developing embryos a high level of expression is confined to the nervous system particularly in the dorsal root ganglia, cranial nerves, and neural retina. The gene is composed of eight exons and is located in the 1q21.3 chromosomal region. A pseudogene has been sequenced and mapped to chromosomal region 13q12. PRUNE protein retains the four characteristic domains of DHH phosphoesterases. The synergism between prune and awdK-pn in Drosophila has led various authors to propose an interaction between these genes. However, such an interaction has never been supported by biochemical data. By using interaction-mating and in vitro co-immunoprecipitation experiments, we show for the first time the ability of human PRUNE to interact with the human homologue of awd protein (nm23-H1). In contrast, PRUNE is impaired in its interaction with nm-23-H1-S120G mutant, a gain-of-function mutation associated with advanced neuroblastoma stages. Consistently, PRUNE and nm23-H1 proteins partially colocalize in the cytoplasm. The data presented are consistent with the view that PRUNE acts as a negative regulator of the nm23-H1 protein. We discuss how PRUNE regulates nm23-H1 protein and postulate possible implications of PRUNE in neuroblastoma progression.

Citing Articles

Neuroimaging in PRUNE1 syndrome: a mini-review of the literature.

Scorrano G, Laura B, Spiaggia R, Basile A, Palmucci S, Foti P Front Neurol. 2024; 14:1301147.

PMID: 38178891 PMC: 10764560. DOI: 10.3389/fneur.2023.1301147.

Generation of Conditional Knockout Alleles for PRUNE-1.

Wu X, Simard L, Ding H Cells. 2023; 12(4).

PMID: 36831191 PMC: 9954577. DOI: 10.3390/cells12040524.

Neurodevelopmental disorder with microcephaly, hypotonia, and variable brain anomalies in a consanguineous Iranian family is associated with a homozygous start loss variant in the PRUNE1 gene.

Agha Gholizadeh M, Mohammadi-Sarband M, Fardanesh F, Garshasbi M BMC Med Genomics. 2022; 15(1):78.

PMID: 35379233 PMC: 8981834. DOI: 10.1186/s12920-022-01228-6.

PRUNE1 c.933G>A synonymous variant induces exon 7 skipping, disrupts the DHHA2 domain, and leads to an atypical NMIHBA syndrome presentation: Case report and review of the literature.

Magyar C, Murdock D, Burrage L, Dai H, Lalani S, Lewis R Am J Med Genet A. 2022; 188(6):1868-1874.

PMID: 35194938 PMC: 11149102. DOI: 10.1002/ajmg.a.62704.

Functional Genomics of PRUNE1 in Neurodevelopmental Disorders (NDDs) Tied to Medulloblastoma (MB) and Other Tumors.

Bibbo F, Sorice C, Ferrucci V, Zollo M Front Oncol. 2021; 11:758146.

PMID: 34745995 PMC: 8569853. DOI: 10.3389/fonc.2021.758146.