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Synchronous activities among neurons in the brain generate emergent network oscillations such as the hippocampal Sharp-wave ripples (SPWRs) that facilitate information processing during memory formation. However, how neurons and circuits are functionally organized to generate oscillations remains unresolved. Biophysical models of neuronal networks can shed light on how thousands of neurons interact in intricate circuits to generate such emergent SPWR network events. Here we developed a large-scale biophysically realistic neural network model of CA1 hippocampus with functionally organized circuit modules containing distinct types of neurons. Model simulations reproduced synaptic, cellular and network aspects of physiological SPWRs. The model provided insights into the role of neuronal types and their microcircuit motifs in generating SPWRs in the CA1 region. The model also suggests experimentally testable predictions including the role of specific neuron types in the genesis of hippocampal SPWRs.
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Synchronized activity in neural circuits, detected as oscillations in the extracellular field potential, has been associated with learning and memory. Neural circuits in the basolateral amygdala (BLA), a mid-temporal lobe structure, generate oscillations in specific frequency bands to mediate emotional memory functions. However, how BLA circuits generate oscillations in distinct frequency bands is not known. Of these, sharp-waves (SWs) are repetitive, brief transitions that contain a low-frequency (<20 Hz) envelope, often coupled with ripples (100-300 Hz), have been associated with memory consolidation. Here, we show that SWs are retained in the BLA ex vivo and generated by local circuits. We demonstrate that an action potential in a chandelier interneuron is sufficient to initiate SWs through local circuits. Using a physiologically constrained model, we show that microcircuits organized as chandelier-interneuron-driven modules reproduce SWs and associated cellular events, revealing a functional role for chandelier interneurons and microcircuits for SW generation.
Assuntos
Potenciais de Ação/fisiologia , Tonsila do Cerebelo/fisiologia , Complexo Nuclear Basolateral da Amígdala/metabolismo , Interneurônios/metabolismo , HumanosRESUMO
Algal productivity in steady-state cultivation systems depends on important factors such as biomass concentration, solids retention time (SRT), and light intensity. Current modeling of algal growth often ignores light distribution in algal cultivation systems and does not consider all these factors simultaneously. We developed a new algal growth model using a first principles approach to incorporate the effect of light intensity on algal growth while simultaneously considering biomass concentration and SRT. We first measured light attenuation (decay) with depth in an indoor algal membrane bioreactor (A-MBR) cultivating Chlorella sp. We then simulated the light decay using a multi-layer approach and correlated the decay with biomass concentration and SRT in model development. The model was calibrated by delineating specific light absorptivity and half-saturation constant to match the algal biomass concentration in the A-MBR operated at a target SRT. We finally applied the model to predict the maximum algal productivity in both indoor and outdoor A-MBRs. The predicted maximum algal productivities in indoor and outdoor A-MBRs were 6.7 g·m-2·d-1 (incident light intensity 5732 lx, SRT approximately 8 d) and 28 g·m-2·d-1 (sunlight intensity 28,660 lx, SRT approximately 4 d), respectively. The model can be extended to include other factors (e.g., water temperature and carbon dioxide bubbling) and such a modeling framework can be applied to full-scale, continuous flow outdoor systems to improve algal productivity.
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Chlorella , Biomassa , Reatores Biológicos , Dióxido de Carbono , TemperaturaRESUMO
Contribution: This paper demonstrates curricular modules that incorporate engineering model-based approaches, including concepts related to circuits, systems, modeling, electrophysiology, programming, and software tutorials that enhance learning in undergraduate neuroscience courses. These modules can also be integrated into other neuroscience courses. Background: Educators in biological and physical sciences urge incorporation of computation and engineering approaches into biology. Model-based approaches can provide insights into neural function; prior studies show these are increasingly being used in research in biology. Reports about their integration in undergraduate neuroscience curricula, however, are scarce. There is also a lack of suitable courses to satisfy engineering students' interest in the challenges in the growing area of neural sciences. Intended Outcomes: (1) Improved student learning in interdisciplinary neuroscience; (2) enhanced teaching by neuroscience faculty; (3) research preparation of undergraduates; and 4) increased interdisciplinary interactions. Application Design: An interdisciplinary undergraduate neuroscience course that incorporates computation and model-based approaches and has both software- and wet-lab components, was designed and co-taught by colleges of engineering and arts and science. Findings: Model-based content improved learning in neuroscience for three distinct groups: 1) undergraduates; 2) Ph.D. students; and 3) post-doctoral researchers and faculty. Moreover, the importance of the content and the utility of the software in enhancing student learning was rated highly by all these groups, suggesting a critical role for engineering in shaping the neuroscience curriculum. The model for cross-training also helped facilitate interdisciplinary research collaborations.
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We developed an interdisciplinary course in computational neuroscience to address the need for students trained in both biological/psychological and quantitative sciences. Increasingly, exposure to advanced math and physics is important to stay on the cutting edge of developments and research in neuroscience. Additionally, the ability to work in multidisciplinary teams will continue to be an asset as the field develops. This course brings together students from biology, psychology, biochemistry, engineering, physics, and mathematics. The course was designed to highlight the importance of math in understanding fundamental neuroscience concepts and to prepare students for professional careers in neuroscience. They learn neurobiology, via a 'biology to model and back again' approach involving wet- and software/modeling-labs, with the latter being the focus of this paper. We presented a subset of the software activities described here at the 2017 Faculty for Undergraduate Neuroscience Workshop.
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OBJECTIVE: To report a novel mechanism suggestive of early ovarian failure secondary to the anti-tumor hedgehog-pathway inhibitor vismodegib. DESIGN: Case report and literature review. SETTING: Academic and private dermatology and fertility practices. PATIENT(S): A 34-year-old nulliparous woman with locally advanced basal cell carcinomas who became amenorrheic while receiving oral therapy with vismodegib. INTERVENTION(S): Physical examination and endocrine evaluation. MAIN OUTCOME MEASURE(S): Elevated follicle-stimulating hormone (FSH) and low estrogen in the setting of a normal anti-Müllerian hormone. RESULT(S): FSH was elevated; estrogen was low. Preantral follicles were detected and anti-Müllerian hormone activity was normal. Menses resumed 5 weeks after cessation of therapy. CONCLUSION(S): Vismodegib, a first-in-class inhibitor of the hedgehog signaling pathway is indicated for advanced basal cell carcinoma and is associated with amenorrhea. The mechanism is unknown; it has some features of ovarian failure but preserves ovarian potential through blockading of FSH-receptor-dependent signal transduction. This effect appears to be rapidly reversible upon cessation of therapy. Vismodegib and related compounds may have potential for a role in intervention for gynecologic and endocrine disorders and in therapy for other issues involving FSH-dependent function.