The more we do, the less we gain? Balancing effort and efficacy in managing the Solidago gigantea invasion

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A Unifying Gravity Framework for Dispersal

Most organisms disperse at some life-history stage, but different research traditions to study dispersal have evolved in botany, zoology, and epidemiology. In this paper, we synthesize concepts, principles, patterns, and processes in dispersal across organisms. We suggest a consistent conceptual framework for dispersal, which utilizes generalized gravity models. This framework will facilitate communication among research traditions, guide the development of dispersal models for theoretical and applied ecology, and enable common representation across taxonomic groups, encapsulating processes at the source and destination of movement, as well as during the intervening relocation process, while allowing each of these stages in the dispersal process to be addressed separately and in relevant detail. For different research traditions, certain parts of the dispersal process are less studied than others (e.g., seed release processes in plants and termination of dispersal in terrestrial and aquatic animals). The generalized gravity model can serve as a unifying framework for such processes, because it captures the general conceptual and formal components of any dispersal process, no matter what the relevant biological timescale involved. We illustrate the use of the framework with examples of passive (a plant), active (an animal), and vectored (a fungus) dispersal, and point out promising applications, including studies of dispersal mechanisms, total dispersal kernels, and spatial population dynamics

A Unifying Gravity Framework for Dispersal

Most organisms disperse at some life-history stage, but different research traditions to study dispersal have evolved in botany, zoology, and epidemiology. In this paper, we synthesize concepts, principles, patterns, and processes in dispersal across organisms. We suggest a consistent conceptual framework for dispersal, which utilizes generalized gravity models. This framework will facilitate communication among research traditions, guide the development of dispersal models for theoretical and applied ecology, and enable common representation across taxonomic groups, encapsulating processes at the source and destination of movement, as well as during the intervening relocation process, while allowing each of these stages in the dispersal process to be addressed separately and in relevant detail. For different research traditions, certain parts of the dispersal process are less studied than others (e.g., seed release processes in plants and termination of dispersal in terrestrial and aquatic animals). The generalized gravity model can serve as a unifying framework for such processes, because it captures the general conceptual and formal components of any dispersal process, no matter what the relevant biological timescale involved. We illustrate the use of the framework with examples of passive (a plant), active (an animal), and vectored (a fungus) dispersal, and point out promising applications, including studies of dispersal mechanisms, total dispersal kernels, and spatial population dynamics

Regulation of PERK Signaling and Leukemic Cell Survival by a Novel Cytosolic Isoform of the UPR Regulator GRP78/BiP

The unfolded protein response (UPR) is an evolutionarily conserved mechanism to allow cells to adapt to stress targeting the endoplasmic reticulum (ER). Induction of ER chaperone GRP78/BiP increases protein folding capacity; as such it represents a major survival arm of UPR. Considering the central importance of the UPR in regulating cell survival and death, evidence is emerging that cells evolve feedback regulatory pathways to modulate the key UPR executors, however, the precise mechanisms remain to be elucidated. Here, we report the fortuitous discovery of GRP78va, a novel isoform of GRP78 generated by alternative splicing (retention of intron 1) and alternative translation initiation. Bioinformatic and biochemical analyses revealed that expression of GRP78va is enhanced by ER stress and is notably elevated in human leukemic cells and leukemia patients. In contrast to the canonical GRP78 which is primarily an ER lumenal protein, GRP78va is devoid of the ER signaling peptide and is cytosolic. Through specific knockdown of endogenous GRP78va by siRNA without affecting canonical GRP78, we showed that GRP78va promotes cell survival under ER stress. We further demonstrated that GRP78va has the ability to regulate PERK signaling and that GRP78va is able to interact with and antagonize PERK inhibitor P58IPK. Our study describes the discovery of GRP78va, a novel cytosolic isoform of GRP78/BiP, and the first characterization of the modulation of UPR signaling via alternative splicing of nuclear pre-mRNA. Our study further reveals a novel survival mechanism in leukemic cells and other cell types where GRP78va is expressed