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由于代谢副产物而在恒化器中共存。

Coexistence in the chemostat as a result of metabolic by-products.

作者信息

Hesseler Julia, Schmidt Julia K, Reichl Udo, Flockerzi Dietrich

机构信息

Department of Mathematics and Physics, Albert-Ludwigs-University, Hermann-Herder-Str. 3, 79104, Freiburg, Germany.

出版信息

J Math Biol. 2006 Oct;53(4):556-84. doi: 10.1007/s00285-006-0012-3. Epub 2006 Jul 4.

Abstract

Classical chemostat models assume that competition is purely exploitative and mediated via a common, limiting and single resource. However, in laboratory experiments with pathogens related to the genetic disease Cystic Fibrosis, species specific properties of production, inhibition and consumption of a metabolic by-product, acetate, were found. These assumptions were implemented into a mathematical chemostat model which consists of four nonlinear ordinary differential equations describing two species competing for one limiting nutrient in an open system. We derive classical chemostat results and find that our basic model supports the competitive exclusion principle, the bistability of the system as well as stable coexistence. The analytical results are illustrated by numerical simulations performed with experimentally measured parameter values. As a variant of our basic model, mimicking testing of antibiotics for therapeutic treatments in mixed cultures instead of pure ones, we consider the introduction of a lethal inhibitor, which cannot be eliminated by one of the species and is selective for the stronger competitor. We discuss our theoretical results in relation to our experimental model system and find that simulations coincide with the qualitative behavior of the experimental result in the case where the metabolic by-product serves as a second carbon source for one of the species, but not the producer.

摘要

经典恒化器模型假设竞争纯粹是剥削性的,并通过一种共同的、有限的单一资源介导。然而,在与遗传性疾病囊性纤维化相关的病原体的实验室实验中,发现了代谢副产物乙酸盐的产生、抑制和消耗的物种特异性特性。这些假设被纳入一个数学恒化器模型,该模型由四个非线性常微分方程组成,描述了在一个开放系统中争夺一种有限营养物质的两个物种。我们推导了经典恒化器结果,发现我们的基本模型支持竞争排斥原理、系统的双稳态以及稳定共存。通过使用实验测量的参数值进行数值模拟来说明分析结果。作为我们基本模型的一个变体,模拟在混合培养而非纯培养中对抗生素进行治疗测试的情况,我们考虑引入一种致命抑制剂,该抑制剂不能被其中一个物种消除,并且对较强的竞争者具有选择性。我们结合实验模型系统讨论了我们的理论结果,发现在代谢副产物作为其中一个物种而非生产者的第二碳源的情况下,模拟结果与实验结果的定性行为一致。

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