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      Mechanisms of animal diapause: recent developments from nematodes, crustaceans, insects, and fish

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          Abstract

          Life cycle delays are beneficial for opportunistic species encountering suboptimal environments. Many animals display a programmed arrest of development (diapause) at some stage(s) of their development, and the diapause state may or may not be associated with some degree of metabolic depression. In this review, we will evaluate current advancements in our understanding of the mechanisms responsible for the remarkable phenotype, as well as environmental cues that signal entry and termination of the state. The developmental stage at which diapause occurs dictates and constrains the mechanisms governing diapause. Considerable progress has been made in clarifying proximal mechanisms of metabolic arrest and the signaling pathways like insulin/Foxo that control gene expression patterns. Overlapping themes are also seen in mechanisms that control cell cycle arrest. Evidence is emerging for epigenetic contributions to diapause regulation via small RNAs in nematodes, crustaceans, insects, and fish. Knockdown of circadian clock genes in selected insect species supports the importance of clock genes in the photoperiodic response that cues diapause. A large suite of chaperone-like proteins, expressed during diapause, protects biological structures during long periods of energy-limited stasis. More information is needed to paint a complete picture of how environmental cues are coupled to the signal transduction that initiates the complex diapause phenotype, as well as molecular explanations for how the state is terminated. Excellent examples of molecular memory in post-dauer animals have been documented in Caenorhabditis elegans. It is clear that a single suite of mechanisms does not regulate diapause across all species and developmental stages.

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          Author and article information

          Journal
          Am J Physiol Regul Integr Comp Physiol
          Am. J. Physiol. Regul. Integr. Comp. Physiol
          ajpregu
          ajpregu
          AJPREGU
          American Journal of Physiology - Regulatory, Integrative and Comparative Physiology
          American Physiological Society (Bethesda, MD )
          0363-6119
          1522-1490
          6 April 2016
          1 June 2016
          1 June 2017
          : 310
          : 11
          : R1193-R1211
          Affiliations
          [1] 1Department of Biological Sciences, Louisiana State University, Baton Rouge, Louisiana;
          [2] 2Departments of Entomology and Evolution, Ecology and Organismal Biology, Ohio State University, Columbus, Ohio;
          [3] 3Department of Biology, Portland State University, Portland, Oregon; and
          [4] 4Department of Biology, McGill University, Montréal, Québec, Canada
          Author notes
          [*]

          All authors contributed equally to this review article.

          Address for reprint requests and other correspondence: S. C. Hand, Dept. of Biological Sciences, Division of Cellular, Developmental and Integrative and Biology, 202 Life Sciences Bldg., Louisiana State Univ., Baton Rouge, LA 70803 (e-mail: shand@ 123456LSU.edu ).
          Article
          PMC4935499 PMC4935499 4935499 R-00250-2015
          10.1152/ajpregu.00250.2015
          4935499
          27053646
          6c50827e-d930-4012-88f3-90744c2f1ac0
          Copyright © 2016 the American Physiological Society
          History
          : 5 June 2015
          : 11 March 2016
          Categories
          Reviews

          metabolism,dormancy,development,diapause,cell cycle
          metabolism, dormancy, development, diapause, cell cycle

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