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Commentary

Ventilator-induced lung injury and mechanotransduction: why should we care?

Mingyao Liu

Author Affiliations

Department of Surgery, Faculty of Medicine, University of Toronto, Toronto, Ontario, Canada

Critical Care 2007, 11:168  doi:10.1186/cc6131


See related research by Li et al., http://ccforum.com/content/11/5/R89


The electronic version of this article is the complete one and can be found online at: http://ccforum.com/content/11/5/168


Published:26 October 2007

© 2007 BioMed Central Ltd

Abstract

Mechanotransduction holds the underlying mechanisms of ventilator-induced lung injury. Research on this subject, however, could be difficult for clinicians, especially when results are controversial. A recent study by Li and co-workers is used as an example, to explain how to critically read literatures related to basic science and how to understand the limitation of experimental studies.

Commentary

As a professor in a clinical department, I am privileged to work with many clinician-investigator trainees. Recently, a new clinical research fellow told me that he had been reading many papers in order to decide which research project he should take. The more he reads, the more confused he feels. Many literatures sound contradictory. How to determine their clinical relevance is a challenge. In fact, this challenge is not only to new fellows, but also to experienced researchers.

In this issue of Critical Care, Dr Li and Dr Quinn and their colleagues published a research article [1] exploring the molecular mechanisms of ventilator-induced lung injury (VILI). I would like to use this interesting article as an example, to lead readers who are not experts in this field through a translational process.

Mechanical force-induced signal transduction (mechano-transduction) is responsible for many physiological processes in lung development [2], in maintaining lung functions [3], and in pathological conditions related to lung diseases, such as asthma, chronic obstructive pulmonary disease (COPD), and acute respiratory distress syndrome (ARDS), especially related to VILI [4]. However, very much like the routes in a city, both "good boys" and "bad boys" drive on the same streets. Many signal transduction pathways are shared by both the injury and repair processes.

Neutrophil recruitment and activation is an important mechanism for lung tissue injury, which is mediated by a group of small molecules, namely chemokines, especially a subgroup of C-X-C chemokines. Interleukin-8 (IL-8) is the best example, which has been shown to be up-regulated by mechanical forces in human lung cells [5]. Rodents do not have the IL-8 gene, but produce macrophage inflammatory protein-2 (MIP-2) and other C-X-C chemokines. Mechanical stretch induced MIP-2 in rat lung cells [6]. Increased MIP-2 in murine lung was observed after high volume ventilation by Dr Li and co-workers [7]. They further questioned that neutrophil migration is mediated by a signal pathway activated by Akt (also called protein kinase B). They used Akt+/- mice, which have lower expression of Akt-1. They also used a chemical inhibitor to prevent the activation of Akt in mice, prior to their exposure to high volume ventilation and/or hyperoxia. Indeed, they demonstrated less lung damage in these experimental settings. This is very exciting, isn't it? However, it is worth mentioning that the Akt pathway is also critically important for proliferation, survival and migration of cell types other than neutrophiles [8]. Inhibition of this pathway in sepsis related lung injury is detrimental [9,10]. The clinical application of this strategy needs to be cautious.

Well, another interesting target is nitric oxide (NO). Based on their recent studies, these researchers suspected that endothelial nitric oxide synthase (eNOS) activation is also part of the mechanisms responsible for VILI. They demonstrated increased phosphorylation of eNOS and also demonstrated that nitric oxide synthase (NOS) inhibitor could attenuate VILI. Increased NOS expression and/or activity have been shown in multiple lung injury models [11] and clinical samples [12]. The outcome of NO related clinical studies, however, is controversial [13], which warns us for further investigation.

As a clinician you may ask why 30 ml/kg of tidal volume was used in this study and you may note that oxygen was used for ventilation. These injurious regimens have been less (if at all) used clinically. Are these experimental data really useful? This is really a good question. First of all, as experimental biologists, we always try to create a condition that can give definite answers. For example, after serum starvation, add a growth factor into the culture medium to initiate a signal transduction, or start mechanical stretch on statically cultured cells. These protocols help us to reveal the potential of a biological stimulus on a particular biological process. This strategy has also been adapted to animal studies. On the other hand, this may also explain why many experimental findings did not translate to good clinical practices. As a bench scientist, one should try to simulate clinical conditions as much as possible. Recently, clinically relevant models have been emphasized [14].

After going through this interesting paper critically, what have we learnt? First, good literature review may lead to proposal of a testable hypothesis in VILI. Secondly, the mechanical force-induced signal transduction by injurious ventilation (high tidal volume and high oxygen tension) could activate pathways that are important for normal functions. Thirdly, blocking the transient activation of these pathways could be beneficial. Last but not the least, awareness of the significance and limitation of experimental data are crucial for our knowledge translation.

Abbreviations

ARDS = acute respiratory distress syndrome; COPD = chronic obstructive pulmonary disease; eNOS = endothelial nitric oxide synthase; IL-8 = Interleukin-8; MIP-2 = macrophage inflammatory protein-2; NO = nitric oxide; NOS = nitric oxide synthase; VILI = ventilator-induced lung injury.

Competing interests

The authors declare that they have no competing interests.

References

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