The human CHRNA7 and CHRFAM7A genes: A review of the genetics, regulation, and function

Sinkus, Melissa L.; Graw, Sharon; Freedman, Robert; Ross, Randal G.; Lester, Henry A.; Leonard, Sherry

doi:10.1016/j.neuropharm.2015.02.006

Cited by 151 publications

(196 citation statements)

References 190 publications

(267 reference statements)

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“…Although the relevance of splice variants in a7 nAChR function still needs to be fully characterized, further efforts have been dedicated to more detailed analysis of the duplicate gene, which corresponds to exons 5-10 of CHRNA7 and is located 1.6 Mb centromeric to CHRNA7, which is now referred to as CHRFAM7A (for a recent detailed review, see Sinkus et al, 2015). The corresponding protein, dup a7, is widely expressed, but in lower levels than a7 nAChRs throughout the body but elevated in peripheral leukocytes (Villiger et al, 2002;Benfante et al, 2011.…”

Section: A the Chrna7 Gene And Its Variantsmentioning

confidence: 99%

“…However, what is missing is the detection of the CHRFAM7A transcript, but as noted in a recent review the similarity of this gene with CHRNA7 renders difficult the query in genome-wide association studies. Nonetheless, CHRFAM7A was recently proposed to be associated with several cognitive deficits (Sinkus et al, 2015).…”

Section: A the Chrna7 Gene And Its Variantsmentioning

confidence: 99%

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Therapeutic Potential ofα7 Nicotinic Acetylcholine Receptors

et al. 2015

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Section: A the Chrna7 Gene And Its Variantsmentioning

confidence: 99%

Section: A the Chrna7 Gene And Its Variantsmentioning

confidence: 99%

Therapeutic Potential ofα7 Nicotinic Acetylcholine Receptors

et al. 2015

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“…As recently reviewed by Costantini et al (2) and Sinkus et al (3), it was almost twenty years later that Gault et al (4) sequenced the human α7nAChR gene on chromosome 15q13-14 and found it to be structurally similar to that of all other species. At the same time, however, they noted the presence of a second, human-specific partially duplicated α7nAChR-like gene that localized 1.6 Mb 5′ upstream from human CHRNA7 (4).…”

Section: Introductionmentioning

confidence: 97%

A Human-Specific α7-Nicotinic Acetylcholine Receptor Gene in Human Leukocytes: Identification, Regulation and the Consequences of CHRFAM7A Expression

Costantini

Dang

Yurchyshyna

et al. 2015

Mol Med

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The human genome contains a variant form of the α7-nicotinic acetylcholine receptor (α7nAChR) gene that is uniquely human. This CHRFAM7A gene arose during human speciation and recent data suggests that its expression alters ligand tropism of the normally homopentameric human α7-AChR ligand-gated cell surface ion channel that is found on the surface of many different cell types. To understand its possible significance in regulating inflammation in humans, we investigated its expression in normal human leukocytes and leukocyte cell lines, compared CHRFAM7A expression to that of the CHRNA7 gene, mapped its promoter and characterized the effects of stable CHRFAM7A overexpression. We report here that CHRFAM7A is highly expressed in human leukocytes but that the levels of both CHRFAM7A and CHRNA7 mRNAs were independent and varied widely. To this end, mapping of the CHRFAM7A promoter in its 5′-untranslated region (UTR) identified a unique 1-kb sequence that independently regulates CHRFAM7A gene expression. Because overexpression of CHRFAM7A in THP1 cells altered the cell phenotype and modified the expression of genes associated with focal adhesion (for example, FAK, P13K, Akt, rho, GEF, Elk1, CycD), leukocyte transepithelial migration (Nox, ITG, MMPs, PKC) and cancer (kit, kitL, ras, cFos cyclinD1, Frizzled and GPCR), we conclude that CHRFAM7A is biologically active. Most surprisingly however, stable CHRFAM7A overexpression in THP1 cells upregulated CHRNA7, which, in turn, led to increased binding of the specific α7nAChR ligand, bungarotoxin, on the THP1 cell surface. Taken together, these data confirm the close association between CHRFAM7A and CHRNA7 expression, establish a biological consequence to CHRFAM7A expression in human leukocytes and support the possibility that this human-specific gene might contribute to, and/or gauge, a human-specific response to inflammation.

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“…Postsynaptically, a7 receptors mediate fast synaptic transmission, and in perisynaptic locations they modulate other inputs to neurons and activate a variety of signaling pathways through volume transmission (Gotti and Clementi, 2004;Jones and Wonnacott, 2004;Dani and Bertrand, 2007;Dickinson et al, 2008;Albuquerque et al, 2009;Sinkus et al, 2015) (Fig. 4).…”

Section: Introductionmentioning

confidence: 99%

“…Significant reduction of a7 in the brain, particularly in the hippocampus, has been reported in Alzheimer disease (Guan et al, 2000;Kadir et al, 2006) and schizophrenic patients (Schaaf, 2014;Dineley et al, 2015). The a7 gene, CHRNA7 on chromosome 15, is genetically linked to multiple disorders with cognitive deficits, including schizophrenia, intellectual disability, bipolar disorder, autism spectrum disorders, attention deficit hyperactivity disorder, epilepsy, Alzheimer disease, and sensory processing deficit (Sinkus et al, 2009(Sinkus et al, , 2015Schaaf, 2014;Dineley et al, 2015;Deutsch et al, 2016). A partial duplication of CHRNA7 resulting in the chimeric gene CHRFAM7A, which is present only in humans, has been associated with schizophrenia (Sinkus et al, 2009;Neri et al, 2012).…”

Section: Introductionmentioning

confidence: 99%

Understanding the Bases of Function and Modulation of α7 Nicotinic Receptors: Implications for Drug Discovery

2016

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The nicotinic acetylcholine receptor (nAChR) belongs to a superfamily of pentameric ligand-gated ion channels involved in many physiologic and pathologic processes. Among nAChRs, receptors comprising the a7 subunit are unique because of their high Ca 21 permeability and fast desensitization. nAChR agonists elicit a transient ion flux response that is further sustained by the release of calcium from intracellular sources. Owing to the dual ionotropic/metabotropic nature of a7 receptors, signaling pathways are activated. The a7 subunit is highly expressed in the nervous system, mostly in regions implicated in cognition and memory and has therefore attracted attention as a novel drug target. Additionally, its dysfunction is associated with several neuropsychiatric and neurologic disorders, such as schizophrenia and Alzheimer's disease. a7 is also expressed in non-neuronal cells, particularly immune cells, where it plays a role in immunity, inflammation, and neuroprotection. Thus, a7 potentiation has emerged as a therapeutic strategy for several neurologic and inflammatory disorders. With unique activation properties, the receptor is a sensitive drug target carrying different potential binding sites for chemical modulators, particularly agonists and positive allosteric modulators. Although macroscopic and singlechannel recordings have provided significant information about the underlying molecular mechanisms and binding sites of modulatory compounds, we know just the tip of the iceberg. Further concerted efforts are necessary to effectively exploit a7 as a drug target for each pathologic situation. In this article, we focus mainly on the molecular basis of activation and drug modulation of a7, key pillars for rational drug design.

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The human CHRNA7 and CHRFAM7A genes: A review of the genetics, regulation, and function

Cited by 151 publications

References 190 publications

Therapeutic Potential ofα7 Nicotinic Acetylcholine Receptors

Therapeutic Potential ofα7 Nicotinic Acetylcholine Receptors

A Human-Specific α7-Nicotinic Acetylcholine Receptor Gene in Human Leukocytes: Identification, Regulation and the Consequences of CHRFAM7A Expression

Understanding the Bases of Function and Modulation of α7 Nicotinic Receptors: Implications for Drug Discovery

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