Resistance to Noise-Induced Hearing Loss in 129S6 and MOLF Mice: Identification of Independent, Overlapping, and Interacting Chromosomal Regions

Street, Valerie A.; Kujawa, Sharon G.; Manichaikul, Ani; Broman, Karl W.; Kallman, Jeremy C.; Shilling, Dustin; Iwata, Ayaka J.; Robinson, Linda C.; Robbins, Carol A.; Li, Jin; Liberman, M. Charles; Tempel, Bruce L.

doi:10.1007/s10162-014-0472-x

Cited by 11 publications

(13 citation statements)

References 36 publications

(16 reference statements)

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“…2; Shao et al 2010;Yazbek et al 2011;DeSantis et al 2013;Kato et al 2014;Winawer et al 2014;Zhu and Matin 2014). The CSSs and congenic strains derived from CSSs have been used to map QTLs and identify causal genetic variants for traits such as body weight, glucose homeostasis, anxiety, hearing loss, bone morphology, blood clotting, liver fibrosis, energy expenditure, seizure susceptibility, among others (Singer et al 2004;Singer 2005;Winawer et al 2007;Gregorová et al 2008;Sa et al 2008;Shao et al 2008;Boell et al 2011;DeSantis et al 2013;Spiezio et al 2014;Street et al 2014). …”

Section: Chromosome Substitution Strains (Csss)mentioning

confidence: 99%

“…For example, a double CSS, which combined substituted Chromosomes 2 and 6, synergistically increased airway hyperresponsiveness (Ackerman et al 2005). Another example involves noise-induced hearing loss in CSSs and congenic strains derived from 129S6/SvEvTac and CBA/CaJ (Street et al 2014). Although QTLs were mapped to Chromosomes 4 and 17 with CSSs, subsequent studies with congenic strains and CSS crosses revealed both inter-and intrachromosomal epistatic interactions that regulated hearing loss.…”

Section: Epistasismentioning

confidence: 99%

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Contrasting genetic architectures in different mouse reference populations used for studying complex traits

Buchner

Nadeau

2015

Genome Res.

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Quantitative trait loci (QTLs) are being used to study genetic networks, protein functions, and systems properties that underlie phenotypic variation and disease risk in humans, model organisms, agricultural species, and natural populations. The challenges are many, beginning with the seemingly simple tasks of mapping QTLs and identifying their underlying genetic determinants. Various specialized resources have been developed to study complex traits in many model organisms. In the mouse, remarkably different pictures of genetic architectures are emerging. Chromosome Substitution Strains (CSSs) reveal many QTLs, large phenotypic effects, pervasive epistasis, and readily identified genetic variants. In contrast, other resources as well as genome-wide association studies (GWAS) in humans and other species reveal genetic architectures dominated with a relatively modest number of QTLs that have small individual and combined phenotypic effects. These contrasting architectures are the result of intrinsic differences in the study designs underlying different resources. The CSSs examine contextdependent phenotypic effects independently among individual genotypes, whereas with GWAS and other mouse resources, the average effect of each QTL is assessed among many individuals with heterogeneous genetic backgrounds. We argue that variation of genetic architectures among individuals is as important as population averages. Each of these important resources has particular merits and specific applications for these individual and population perspectives. Collectively, these resources together with high-throughput genotyping, sequencing and genetic engineering technologies, and information repositories highlight the power of the mouse for genetic, functional, and systems studies of complex traits and disease models.

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Section: Chromosome Substitution Strains (Csss)mentioning

confidence: 99%

Section: Epistasismentioning

confidence: 99%

Contrasting genetic architectures in different mouse reference populations used for studying complex traits

Buchner

Nadeau

2015

Genome Res.

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“…The phl1 locus on proximal Chr 17 and the ahl3 locus on distal Chr 17 are in the same regions that were shown on 129S6 mouse to have nr1 and nr6 loci, respectively (Street et al 2014). In light of this evidence, we speculated whether the AHL phenotype in 129S6 mice is genetically linked to the NR loci of Chr 17.…”

Section: Introductionmentioning

confidence: 87%

“…The strongest statistical association with NR was found on Chr 17, indicating that genes in these regions are most likely to contribute to the NR phenotype. Chr 17 was linked to two loci, nr1 on proximal Chr 17 (between markers D17Mit143-D17Mit100) and nr6 on distal Chr 17 (between markers D17Mit119-D17Mit1) (Street et al 2014). Independently, other research has shown that these genomic regions were also associated to other AHL genes (Mashimo et al 2006;Nemoto et al 2004).…”

Section: Introductionmentioning

confidence: 95%

“…Inbred mice strains with age-related hearing loss (AHL) are commonly used to understand the genetic basis of presbycusis. The 129S6 inbred mouse is a unique model of presbycusis in that it has early-onset AHL starting by 1 month of age, as well as having a remarkable resistance to noise-induced hearing loss (NIHL) (Yoshida et al 2000;Rosowski et al 2003;Ohlemiller and Gagnon 2004;Street et al 2014). Other known mice with AHL have a predisposition for NIHL, suggesting these traits are associated (Erway et al 1996;Davis et al 2001;Vázquez et al 2004).…”

Section: Introductionmentioning

confidence: 95%

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A Chromosome 17 Locus Engenders Frequency-Specific Non-Progressive Hearing Loss that Contributes to Age-Related Hearing Loss in Mice

Peguero

Tempel

2015

JARO

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The 129S6/SvEvTac (129S6) inbred mouse is known for its resistance to noise-induced hearing loss (NIHL). However, less is understood of its unique age-related hearing loss (AHL) phenotype and its potential relationship with the resistance to NIHL. Here, we studied the physiological characteristics of hearing loss in 129S6 and asked if noise resistance (NR) and AHL are genetically linked to the same chromosomal region. We used auditory brainstem response (ABR) and distortion product otoacoustic emissions (DPOAE) to examine hearing sensitivity between 1 and 13 months of age of recombinant-inbred (congenic) mice with an NR phenotype. We identified a region of proximal chromosome (Chr) 17 (D17Mit143-D17Mit100) that contributes to a sensory, non-progressive hearing loss (NPHL) affecting exclusively the high-frequencies (>24 kHz) and maps to the nr1 locus on Chr 17. ABR experiments showed that 129S6 and CBA/CaJ F1 (CBACa) hybrid mice exhibit normal hearing, indicating that the hearing loss in 129S6 mice is inherited recessively. An allelic complementation test between the 129S6 and 101/H (101H) strains did not rescue hearing loss, suggesting genetic allelism between the nphl and phl1 loci of these strains, respectively. The hybrids had a milder hearing loss than either parental strain, which indicate a possible interaction with other genes in the mouse background or a digenic interaction between different genes that reside in the same genomic region. Our study defines a locus for nphl on Chr 17 affecting frequencies greater than 24 kHz.

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Pathology and mechanisms of cochlear aging

Keithley

2019

J of Neuroscience Research

137

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Presbycusis, or age‐related hearing loss (ARHL), occurs in most mammals with variations in the age of onset, rate of decline, and magnitude of degeneration in the central nervous system and inner ear. The affected cochlear structures include the stria vascularis and its vasculature, spiral ligament, sensory hair cells and auditory neurons. Dysfunction of the stria vascularis results in a reduced endocochlear potential. Without this potential, the cochlear amplification provided by the electro‐motility of the outer hair cells is insufficient, and a high‐frequency hearing‐loss results. Degeneration of the sensory cells, especially the outer hair cells also leads to hearing loss due to lack of amplification. Neuronal degeneration, another hallmark of ARHL, most likely underlies difficulties with speech discrimination, especially in noisy environments. Noise exposure is a major cause of ARHL. It is well‐known to cause sensory cell degeneration, especially the outer hair cells at the high frequency end of the cochlea. Even loud, but not uncomfortable, sound levels can lead to synaptopathy and ultimately neuronal degeneration. Even in the absence of a noisy environment, aged cells degenerate. This pathology most likely results from damage to mitochondria and contributes to degenerative changes in the stria vascularis, hair cells, and neurons. The genetic underpinnings of ARHL are still unknown and most likely involve various combinations of genes. At present, the only effective strategy for reducing ARHL is prevention of noise exposure. If future strategies can improve mitochondrial activity and reduce oxidative damage in old age, these should also bring relief.

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Resistance to Noise-Induced Hearing Loss in 129S6 and MOLF Mice: Identification of Independent, Overlapping, and Interacting Chromosomal Regions

Cited by 11 publications

References 36 publications

Contrasting genetic architectures in different mouse reference populations used for studying complex traits

Contrasting genetic architectures in different mouse reference populations used for studying complex traits

A Chromosome 17 Locus Engenders Frequency-Specific Non-Progressive Hearing Loss that Contributes to Age-Related Hearing Loss in Mice

Pathology and mechanisms of cochlear aging

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