Counting the Zinc-Proteins Encoded in the Human Genome

Andreini, Claudia; Banci, Lucia; Bertini, Ivano; Rosato, Antonio

doi:10.1021/pr050361j

Cited by 899 publications

(709 citation statements)

References 36 publications

(56 reference statements)

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“…With the identification of a zinc finger protein that displays poly(A) binding, the repertoire of this family of proteins has expanded. Given that zinc finger domains are one of the most abundant domains found in the human genome (42), this finding raises the possibility that there are additional pro- Fig. 3.…”

Section: Discussionmentioning

confidence: 99%

Recognition of polyadenosine RNA by zinc finger proteins

Kelly¹,

Pabit

Kitchen

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

121

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Messenger RNA transcripts are coated from cap to tail with a dynamic combination of RNA binding proteins that process, package, and ultimately regulate the fate of mature transcripts. One class of RNA binding proteins essential for multiple aspects of mRNA metabolism consists of the poly(A) binding proteins. Previous studies have concentrated on the canonical RNA recognition motif-containing poly(A) binding proteins as the sole family of poly(A)-specific RNA binding proteins. In this study, we present evidence for a previously uncharacterized poly(A) recognition motif consisting of tandem CCCH zinc fingers. We have probed the nucleic acid binding properties of a yeast protein, Nab2, that contains this zinc finger motif. Results of this study reveal that the seven tandem CCCH zinc fingers of Nab2 specifically bind to polyadenosine RNA with high affinity. Furthermore, we demonstrate that a human protein, ZC3H14, which contains CCCH zinc fingers homologous to those found in Nab2, also specifically binds polyadenosine RNA. Thus, we propose that these proteins are members of an evolutionarily conserved family of poly(A) RNA binding proteins that recognize poly(A) RNA through a fundamentally different mechanism than previously characterized RNA recognition motif-containing poly(A) binding proteins.CCCH zinc finger ͉ poly(A) binding protein ͉ RNA binding

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Section: Discussionmentioning

confidence: 99%

Recognition of polyadenosine RNA by zinc finger proteins

Kelly¹,

Pabit

Kitchen

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

121

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“…Zinc is the second most abundant transition metal in living organisms and is thought to complex with ϳ10% of the human proteome (21). It has catalytic, structural, or regulatory roles in proteins that are involved in diverse biological processes (22).…”

Section: Znmentioning

confidence: 99%

Probing the Structural Basis of Zn2+ Regulation of the Epithelial Na+ Channel

Chen

Winarski

Myerburg

et al. 2012

Journal of Biological Chemistry

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“…Although worldwide research on genetic variation that requires a different RDA or UL is still in progress, several genes and alleles have been suggested to affect nutrient utilization, including genes involved in the metabolism of folate and vitamin B-12 [60,62,91], lipids [61,74] alcohol [20], lactose [142], iron [46,77] and zinc [31,97]. In the context of healthy lifespan and longevity, nutrigenetic and nutrigenomic implications around this last nutrient (zinc) appear very important taking into account that: (1) RDA (11 mg/day for men and 8 mg/day for women) and UL (40 mg/day for adults) for zinc are very close [50]; (2) About 10% of the human proteome consists in potential Znbinding proteins [5]; (3) Proteins devoted to Zn transport (ZnT) and buffering, most of which display functional polymorphic sites, include at least ten members of the ZnT family [134], 15 members of the ZIP family (i.e. Zn-regulated metal transporter, iron-regulated metal transporterlike protein) [36,134] and ten distinct isoforms of MT [150]; 4) zinc is an essential micronutrient strictly involved in regulating gene expression [35], inflammatory response [63,124] and antioxidant activity [125].…”

Section: Human Genes and Longevitymentioning

confidence: 99%

Zinc–gene interaction related to inflammatory/immune response in ageing

Mocchegiani

Malavolta

2008

Genes Nutr

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The pivotal role played by zinc-gene interaction in affecting some relevant cytokines (IL-6 and TNF-a) and heat shock proteins (HSP70-2) in ageing, successful ageing (nonagenarians) and the most common age-related diseases, such as atherosclerosis and infections, is now recognized. The polymorphisms of genes codifying proteins related to the inflammation are predictive on one hand in longevity, on the other hand they are associated with atherosclerosis or severe infections. Since the health lifespan has a strong genetic component, which in turn also affected by nutritional factors like zinc, the association of these polymorphisms with innate immune response, zinc ion bioavailability and Metallothioneins (MT) homeostasis is an useful tool to unravel the role played by zinc-gene interactions in longevity, especially due to the inability of MT in zinc release in ageing and chronic inflammation. In ageing, this last fact leads to depressed innate immune response for host defence. In contrast, in very old age the inflammation is lower with subsequent more zinc ion bioavailability, less MT gene expression and satisfactory innate immunity. Therefore, the zinc-gene (IL-6, TNF-a, Hsp70-2) interactions, via MT homeostasis, are crucial to achieve successful ageing. Human genes and longevityAgeing is a universal phenomenon that affects nearly all of animal species. According to Helfand and Rogina [69], ageing can be characterized as: (1) an inevitable consequence of being a multicellular organism; (2) associated with a random, passive decline in function; (3) leading to a global loss of homeostasis over time and (4) mortality increasing with ageing. Evolutionary studies on ageing have drawn the attention on the importance of the genetic mechanisms involved in somatic maintenance and repair that secure longevity [82]. Evidence from model organisms has indicated that subtle variation in the genes can dramatically influence lifespan. However, findings on potential candidate genetic mechanisms determining ageing and lifespan in model organisms are far to explain variations in human populations because phenotypes are critically dependent on the setting in which genes are expressed, while laboratory conditions and modern environments are markedly dissimilar [86]. Genetic analysis of human ageing is mainly approached by searching the genetic basis of susceptibility to major geriatric disorders or the allelic contributions to exceptionally long life span. It is just thanks to these last studies in centenarians populations that several candidate longevity genes or pathways including PON1 [19,130], IGF1/insulin pathway [84,120], elements of lipid metabolism [12], stress response [34] and inflammatory response have been identified [53].Genes related to inflammation and stress response, in particular the pro-inflammatory cytokines IL-1, IL-6, TNFalpha, the anti-inflammatory cytokine IL-10, the HSP70 chaperones and the regulators of trace elements homeostasis, metallothioneins (MT), seem particularly relevant taking into accoun...

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Counting the Zinc-Proteins Encoded in the Human Genome

Cited by 899 publications

References 36 publications

Recognition of polyadenosine RNA by zinc finger proteins

Recognition of polyadenosine RNA by zinc finger proteins

Probing the Structural Basis of Zn2+ Regulation of the Epithelial Na+ Channel

Zinc–gene interaction related to inflammatory/immune response in ageing

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