The evolutionarily conserved transcription factor PRDM12 controls sensory neuron development and pain perception

Nagy, Vanja; Cole, Tiffany; Campenhout, Claude Van; Khoung, Thang M; Leung, Calvin; Vermeiren, Simon; Novatchkova, Maria; Wenzel, D.; Cikes, Domagoj; Polyansky, Anton A.; Kozieradzki, I.; Meixner, Arabella; Bellefroid, Éric; Neely, G. Gregory; Penninger, Josef

doi:10.1080/15384101.2015.1036209

Cited by 43 publications

(56 citation statements)

References 49 publications

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“…The encoded protein is an extracellular peptidase that specifically cleaves and inactivates the neuropeptide thyrotropin-releasing hormone (Bauer et al, 1999). Concurring with this, knockdown of TRHDE in Drosophila sensory neurons is known to result in altered cellular morphology, impaired nociception and the sensory response to (potentially) harmful stimuli (Nagy et al, 2015). In our study, carriers of the minor allele showed a slower increase of cerebellum white matter, followed by reduced decline in older age (Supplementary Figure S5).…”

Section: Age-dependent Associations With Brain-structural Change Ratessupporting

confidence: 50%

Age-dependent genetic variants associated with longitudinal changes in brain structure across the lifespan

Brouwer¹,

Haren²,

Forti³

et al. 2020

Preprint

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We identified common genetic variants associated with the rate of brain development and aging, in longitudinal MRI scans worldwide. AbstractHuman brain structure changes throughout our lives. Altered brain growth or rates of decline are implicated in a vast range of psychiatric, developmental, and neurodegenerative diseases. While heritable, specific loci in the genome that influence these rates are largely unknown. Here, we sought to find common genetic variants that affect rates of brain growth or atrophy, in the first genome-wide association analysis of longitudinal changes in brain morphology across the lifespan. Longitudinal magnetic resonance imaging data from 10,163 individuals aged 4 to 99 years, on average 3.5 years apart, were used to compute rates of morphological change for 15 brain structures. We discovered 5 genome-wide significant loci and 15 genes associated with brain structural changes. Most individual variants exerted age-dependent effects. All identified genes are expressed in fetal and adult brain tissue, and some exhibit developmentally regulated expression across the lifespan. We demonstrate genetic overlap with depression, schizophrenia, cognitive functioning, height, body mass index and smoking. Several of the discovered loci are implicated in early brain development and point to involvement of metabolic processes. Gene-set findings also implicate immune processes in the rates of brain changes. Taken together, in the world's largest longitudinal imaging genetics dataset we identified genetic variants that alter agedependent brain growth and atrophy throughout our lives. a Position based on build hg19. Study-wide significant hits are displayed in bold. *This gene also showed a genome-wide significant quadratic age effect. The most parsimonious model is listed in this table.Genome-wide significant gene sets based on gene ontology. Study-wide significant gene sets are displayed in bold. a See Supplementary Table S9 for genes included in the gene set. Genes included in GO_INTERLEUKIN_1_RECEPTOR_ACTIVITY and GO_RESPONSE_TO_INTERLEUKIN_2 do not overlap.

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Section: Age-dependent Associations With Brain-structural Change Ratessupporting

confidence: 50%

Age-dependent genetic variants associated with longitudinal changes in brain structure across the lifespan

Brouwer¹,

Haren²,

Forti³

et al. 2020

Preprint

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“…By contrast, our data indicate that Xenopus or mouse Prdm12 promotes En1 + V1 INs when overexpressed in the frog or chick embryo. Human PRDM12 also induces en1 when overexpressed in the frog (Nagy et al, 2015). The reasons for this functional difference between zebrafish and tetrapode vertebrate Prdm12 are unclear and remain to be determined.…”

Section: Discussion Prdm12 Function In Vertebrate V1 In Specificationmentioning

confidence: 99%

“…Prdm12 is highly conserved during evolution (Nagy et al, 2015), and we identified orthologous sequences in the chicken and the cephalochordate amphioxus (Branchiostoma lanceolatum), a basal chordate (supplementary material Fig. S1).…”

Section: Cloning and Expression Of Xenopus Chicken And Amphioxus Prdmentioning

confidence: 99%

“…In a recent study, different homozygous mutations have been identified throughout Prdm12 that all abrogates its histone-modifying activity (Chen et al, 2015). Some of these mutated forms of Prdm12, when overexpressed in Xenopus, exhibit an impaired activity to induce en1 (Nagy et al, 2015). It remains to be tested whether the amphioxus Prdm12 is inactive because of its impaired histonemodifying potential.…”

Section: Prdm12 Mechanism Of Action In V1 Insmentioning

confidence: 99%

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Prdm12 specifies V1 interneurons through cross-repressive interactions with Dbx1 and Nkx6 genes in Xenopus

et al. 2015

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V1 interneurons are inhibitory neurons that play an essential role in vertebrate locomotion. The molecular mechanisms underlying their genesis remain, however, largely undefined. Here, we show that the transcription factor Prdm12 is selectively expressed in p1 progenitors of the hindbrain and spinal cord in the frog embryo, and that a similar restricted expression profile is observed in the nerve cord of other vertebrates as well as of the cephalochordate amphioxus. Using frog, chick and mice, we analyzed the regulation of Prdm12 and found that its expression in the caudal neural tube is dependent on retinoic acid and Pax6, and that it is restricted to p1 progenitors, due to the repressive action of Dbx1 and Nkx6-1/2 expressed in the adjacent p0 and p2 domains. Functional studies in the frog, including genomewide identification of its targets by RNA-seq and ChIP-Seq, reveal that vertebrate Prdm12 proteins act as a general determinant of V1 cell fate, at least in part, by directly repressing Dbx1 and Nkx6 genes. This probably occurs by recruiting the methyltransferase G9a, an activity that is not displayed by the amphioxus Prdm12 protein. Together, these findings indicate that Prdm12 promotes V1 interneurons through cross-repressive interactions with Dbx1 and Nkx6 genes, and suggest that this function might have only been acquired after the split of the vertebrate and cephalochordate lineages.

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“…Ген PRDM12 кодирует эпигенетический регулятор, который является ключевым в процессе мейоза, участвует в нейрогенезе и влияет на свойства нервных клеток [18,24]. PRDM12 необходим для разви-тия сенсорного нейрона и восприятия боли [17,[25][26][27]. Было показано участие гена PRDM12 в модуляции ноцицепторов и сенсорных нейронов у эмбрионов Xenopus [17].…”

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Analysis of the association of the PRDM12 gene with pain sensitivity in individuals with psychoactive substance dependence

Poltavskaya

Савочкина

2020

RJTAO

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Ранняя диагностика предрасположенности к употреблению психоактивных веществ (ПАВ) и формированию зависимости является актуальной проблемой аддиктологии. В развитии зависимости от ПАВ задействована система вознаграждения, которая также играет ключевую роль в модуляции ноцицепции. PRDM12, связанный с врожденной нечувствительностью к боли, участвует в нейрогенезе и влияет на свойства нервных клеток. Цель исследования-сравнительная оценка болевой чувствительности при психических и поведенческих расстройствах, вызванных употреблением ПАВ, у здоровых лиц и у лиц с эпизодическим употреблением ПАВ в зависимости от генотипа rs10121864 гена PRDM12. Пациенты и методы. Обследовано 103 пациента с зависимостью от ПАВ (F1x.2), 114 условно здоровых лиц (контроль) и 36 лиц, эпизодически употребляющих ПАВ (группа риска). Порог болевой чувствительности и переносимость боли определяли методом тензоалгометрии; субъективную оценку болевых порогов-с помощью визуальной аналоговой шкалы. Выполнено генотипирование по полиморфизму rs10121864 гена PRDM12.

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The evolutionarily conserved transcription factor PRDM12 controls sensory neuron development and pain perception

Cited by 43 publications

References 49 publications

Age-dependent genetic variants associated with longitudinal changes in brain structure across the lifespan

Age-dependent genetic variants associated with longitudinal changes in brain structure across the lifespan

Prdm12 specifies V1 interneurons through cross-repressive interactions with Dbx1 and Nkx6 genes in Xenopus

Analysis of the association of the PRDM12 gene with pain sensitivity in individuals with psychoactive substance dependence

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