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Mus musculus enters a torpid state in response to caloric restriction in sub-thermoneutral ambient temperatures. This torpid state is characterized by an adaptive and controlled decrease in metabolic rate, heart rate, body temperature, and activity. Previous research has identified the paraventricular nucleus (PVN) within the hypothalamus, a region containing oxytocin neurons, as a location that is active during torpor onset. We hypothesized that oxytocin neurons within the PVN are part of this neural circuit and that activation of oxytocin neurons would deepen and lengthen torpor bouts. We report that activation of oxytocin neurons alone is not sufficient to induce a torpor-like state in the fed mouse, with no significant difference in body temperature or heart rate upon activation of oxytocin neurons. However, we found that activation of oxytocin neurons prior to the onset of daily torpor both deepens and lengthens the subsequent bout, with a 1.7 ± 0.4 °C lower body tempera- ture and a 135 ± 32 min increase in length. We therefore conclude that oxytocin neurons are involved in the neural circuitry controlling daily torpor in the mouse. 

The parabrachial nucleus (PBN) is a major hub that receives sensory information from both internal and external environments. Specific populations of PBN neurons are involved in behaviors including food and water intake, nociceptive responses, breathing regulation, as well as learning and responding appropriately to threatening stimuli. However, it is unclear how many PBN neuron populations exist and how different behaviors may be encoded by unique signaling molecules or receptors. Here we provide a repository of data on the molecular identity, spatial location, and projection patterns of dozens of PBN neuron subclusters. Using single-cell RNA sequencing, we identified 21 subclusters of neurons in the PBN and neighboring regions. Multiplexed in situ hybridization showed many of these subclusters are enriched within specific PBN subregions with scattered cells in several other regions. We also provide detailed visualization of the axonal projections from 21 Cre-driver lines of mice. These results are all publicly available for download and provide a foundation for further interrogation of PBN functions and connections. 

Data preprocessing is an integral step prior to analyzing data in psychological science, with implications for its potentially guiding policy. This article reports how psychological researchers address data preprocessing or quality concerns, with a focus on aberrant responses and missing data in self-report measures. 240 articles were sampled from four journals: Psychological Science, Journal of Personality and Social Psychology, Developmental Psychology, and Abnormal Psychology from 2012 to 2018. Nearly half of the studies did not report any missing data treatment (111/240; 46.25%), and if they did, the most common approach was listwise deletion (71/240; 29.6%). Studies that remove data due to missingness removed, on average, 12% of the sample. Likewise, most studies do not report any aberrant responses (194/240; 80%), but if they did, they classified 4% of the sample as suspect. Most studies are either not transparent enough about their data preprocessing steps or may be leveraging suboptimal procedures. Recommendations can improve transparency and data quality. 

Food intake behavior is regulated by a network of appetite-inducing and appetite-suppressing neuronal populations throughout the brain. The parasubthalamic nucleus (PSTN), a relatively unexplored population of neurons in the posterior hypothalamus, has been hypothesized to regulate appetite due to its connectivity with other anorexigenic neuronal populations and because these neurons express Fos, a marker of neuronal activation, following a meal. However, the individual cell types that make up the PSTN are not well characterized, nor are their functional roles in food intake behavior. Here, we identify and distinguish between two discrete PSTN subpopulations, those that express tachykinin-1 (PSTN Tac1 neurons) and those that express corticotropin-releasing hormone (PSTN CRH neurons), and use a panel of genetically encoded tools in mice to show that PSTN Tac1 neurons play an important role in appetite suppression. Both subpopulations increase activity following a meal and in response to administration of the anorexigenic hormones amylin, cholecystokinin (CCK), and peptide YY (PYY). Interestingly, chemogenetic inhibition of PSTN Tac1 , but not PSTN CRH neurons, reduces the appetite-suppressing effects of these hormones. Consistently, optogenetic and chemogenetic stimulation of PSTN Tac1 neurons, but not PSTN CRH neurons, reduces food intake in hungry mice. PSTN Tac1 and PSTN CRH neurons project to distinct downstream brain regions, and stimulation of PSTN Tac1 projections to individual anorexigenic populations reduces food consumption. Taken together, these results reveal the functional properties and projection patterns of distinct PSTN cell types and demonstrate an anorexigenic role for PSTN Tac1 neurons in the hormonal and central regulation of appetite. 

We report the influence of side chain hydrolysis on the evolution of nanoscale structure in thin films fabricated by the reactive layer-by-layer (LbL) assembly of branched poly(ethylenimine) (PEI) and poly(2-vinyl-4,4-dimethylazlactone) (PVDMA). LbL assembly of PEI and PVDMA generally leads to the linear growth of thin, smooth films. However, assembly using PVDMA containing controlled degrees of side chain hydrolysis leads to the growth of thicker films that exhibit substantial nanoscale roughness, porosity, and have resulting physicochemical behaviors (e.g., superhydrophobicity) that are similar to those of some thicker PEI/PVDMA coatings reported in past studies. Our results reveal that the degree of PVDMA partial hydrolysis (or carboxylic acid group content) influences the extent to which complex film features develop, suggesting that ion-pairing interactions between hydrolyzed side chains and amines in PEI promote the evolution of bulk and surface morphology. Additional experiments demonstrate that these features likely arise from polymer/polymer interactions at the surfaces of the films during assembly, and not from the formation and deposition of solution-phase polymer aggregates. When combined, our results suggest that nanoporous structures and rough features observed in past studies likely arise, at least in part, from some degree of adventitious side chain hydrolysis in the PVDMA used for film fabrication. Our results provide useful insight into molecular-level features that govern the growth and structures of these reactive materials, and provide a framework to promote nanoscale morphology reliably and reproducibly. The principles and tools reported here should prove useful for further tuning the porosities and tailoring the physicochemical behaviors of these reactive coatings in ways that are important in applied contexts.