Values of integration between lipidomics and clinical phenomes in patients with acute lung infection, pulmonary embolism, or acute exacerbation of chronic pulmonary diseases: a preliminary study

Gao, Danyan; Zhang, Linlin; Song, Dongli; Lv, Jiapei; Wang, Linyan; Zhou, Shuang; Li, Yanjun; Zeng, Tao; Zeng, Yiming; Zhang, Jiaqiang; Wang, Xiangdong

doi:10.1186/s12967-019-1898-z

Cited by 20 publications

(30 citation statements)

References 29 publications

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“…We introduced clinical phenomics into trans-omics to evaluate network nodules cross lipidomic and phenomic layers and define phenome-specific lipid panels and lipid-specific phenome groups in acute lung injury patients with or without infections and with or without chronic diseases, as well as in patients with lung cancer subtypes. 8,15,17 To gather our present and previous studies, we found that the variation of trans-omic profiles in patients was TA B L E 8 Lipid elements significantly elevated or declined alone in lung cancer patients survived or nonsurvived (more than twofold), respectively, as compared with healthy control (P-values) more obvious, uncontrolled, and irregular due to the complex and comprehensive influencing factors in clinical practice and measurements. We also found that the integrated panel appeared lung cancer subtype-specific network and the construction to show statistical correlations and mechanistic molecular interactions between lipid metabolisms and phenome appearances in patients with lung cancer.…”

Section: Discussionmentioning

confidence: 91%

“…[19][20][21][22] Clinical phenomes were furthermore integrated with lipidomic profiles in patients with pulmonary embolism, acute pneumonia, and acute exacerbation of chronic obstructive pulmonary diseases, based on clinical trans-omics principle. 15 Lipidomic profiles difference between health and lung cancer has been defined and it depends upon methodologies of measurement and analysis, sample preparations and sources, and patient populations and status. 8 For example, serum levels of lysoPC (C26:0 and C26:1) and PC (C42:4 and C34:4) were different between stage I NSCLC and healthy patients.…”

Section: Discussionmentioning

confidence: 99%

“…About 200 µL plasma was collected into a glass tube, into which 10 µL internal standard was added and then 5 mL of methanol:chloroform:formic acid (10:10:1), as reported previously. 3,15 This mixture was incubated at -20 • C overnight after vigorous shaking. Two milliliters of Hajra's reagent (0.2 M H 3 PO 4 , 1 M KCl) were dropped, blended, and centrifuged at 3000 rpm for 5 min.…”

Section: Lipid Extraction For Mass Spectrometry Analysismentioning

confidence: 99%

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Trans‐omic profiling between clinical phenoms and lipidomes among patients with different subtypes of lung cancer

Zhu

Zhang

et al. 2020

Clinical & Translational Med

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Lung cancer has high mortality, often accompanied with systemic metabolic disorders. The present study aimed at defining values of trans‐nodules cross‐clinical phenomic and lipidomic network layers in patients with adenocarcinoma (ADC), squamous cell carcinomas, or small cell lung cancer (SCLC). We measured plasma lipidomic profiles of lung cancer patients and found that altered lipid panels and concentrations varied among lung cancer subtypes, genders, ages, stages, metastatic status, nutritional status, and clinical phenome severity. It was shown that phosphatidylethanolamine elements (36:2, 18:0/18:2, and 18:1/18:1) were SCLC specific, whereas lysophosphatidylcholine (20:1 and 22:0 sn‐position‐1) and phosphatidylcholine (19:0/19:0 and 19:0/21:2) were ADC specific. There were statistically more lipids declined in male, <60 ages, late stage, metastasis, or body mass index < 22 . Clinical trans‐omics analyses demonstrated that one phenome in lung cancer subtypes might be generated from multiple metabolic pathways and metabolites, whereas a metabolic pathway and metabolite could contribute to different phenomes among subtypes, although those needed to be furthermore confirmed by bigger studies including larger population of patients in multicenters. Thus, our data suggested that trans‐omic profiles between clinical phenomes and lipidomes might have the value to uncover the heterogeneity of lipid metabolism among lung cancer subtypes and to screen out phenome‐based lipid panels as subtype‐specific biomarkers.

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Section: Discussionmentioning

confidence: 91%

Section: Discussionmentioning

confidence: 99%

Section: Lipid Extraction For Mass Spectrometry Analysismentioning

confidence: 99%

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Trans‐omic profiling between clinical phenoms and lipidomes among patients with different subtypes of lung cancer

Zhu

Zhang

et al. 2020

Clinical & Translational Med

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“…Lipidomics has also been utilized to identify lipid profile differences between healthy and diseased human patients. For example, blood plasma from patients with diseases, such as acute lung infections, pulmonary embolism, or acute exacerbation of the chronic pulmonary disease, had a more than 2-fold increase in various lipids compared to healthy patients (109). Lipidomics and liquid chromatography-mass spectrometry may be used to diagnose subclinical coronary artery disease (110) determined that patients with severe coronary calcification tended to have greater levels of monounsaturated triacylglycerols and saturated triacylglycerols.…”

Section: Lipidomic Techniques and Applicationsmentioning

confidence: 99%

Advancing Semen Evaluation Using Lipidomics

et al. 2021

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Developing a deeper understanding of biological components of sperm is essential to improving cryopreservation techniques and reproductive technologies. To fully ascertain the functional determinants of fertility, lipidomic methods have come to the forefront. Lipidomics is the study of the lipid profile (lipidome) within a cell, tissue, or organism and provides a quantitative analysis of the lipid content in that sample. Sperm cells are composed of various lipids, each with their unique contribution to the overall function of the cell. Lipidomics has already been used to find new and exciting information regarding the fatty acid content of sperm cells from different species. While the applications of lipidomics are rapidly evolving, gaps in the knowledge base remain unresolved. Current limitations of lipidomics studies include the number of available samples to analyze and the total amount of cells within those samples needed to detect changes in the lipid profiles across different subjects. The information obtained through lipidomics research is essential to systems and cellular biology. This review provides a concise analysis of the most recent developments in lipidomic research. This scientific resource is important because these developments can be used to not only combat the reproductive challenges faced when using cryopreserved semen and artificial reproductive technologies in livestock such as cattle, but also other mammals, such as humans or endangered species.

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“…Despite improvements in clinical management, mortality remains high and there is no specific treatment, nor are there universally agreed-upon biomarkers for survival and outcome in ARDS. Different types of acute lung diseases have distinct lipid profiles (73) and lipid mediators may represent useful prognostic markers in critically ill patients. LTB4 correlates with lung-injury severity and outcome in patients with ARDS (64,65) and higher pro-inflammatory mediators like PGF2a and selected pro-resolving mediators like 10S,17S-diHDHA were predictive of ARDS development in patients with sepsis (61).…”

Section: Acute Respiratory Distress Syndrome (Ards)mentioning

confidence: 99%

Lipid Mediators in Critically Ill Patients: A Step Towards Precision Medicine

2020

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A dysregulated response to systemic inflammation is a common pathophysiological feature of most conditions encountered in the intensive care unit (ICU). Recent evidence indicates that a dysregulated inflammatory response is involved in the pathogenesis of various ICU-related disorders associated with high mortality, including sepsis, acute respiratory distress syndrome, cerebral and myocardial ischemia, and acute kidney injury. Moreover, persistent or non-resolving inflammation may lead to the syndrome of persistent critical illness, characterized by acquired immunosuppression, catabolism and poor long-term functional outcomes. Despite decades of research, management of many disorders in the ICU is mostly supportive, and current therapeutic strategies often do not take into account the heterogeneity of the patient population, underlying chronic conditions, nor the individual state of the immune response. Fatty acid-derived lipid mediators are recognized as key players in the generation and resolution of inflammation, and their signature provides specific information on patients’ inflammatory status and immune response. Lipidomics is increasingly recognized as a powerful tool to assess lipid metabolism and the interaction between metabolic changes and the immune system via profiling lipid mediators in clinical studies. Within the concept of precision medicine, understanding and characterizing the individual immune response may allow for better stratification of critically ill patients as well as identification of diagnostic and prognostic biomarkers. In this review, we provide an overview of the role of fatty acid-derived lipid mediators as endogenous regulators of the inflammatory, anti-inflammatory and pro-resolving response and future directions for use of clinical lipidomics to identify lipid mediators as diagnostic and prognostic markers in critical illness.

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Values of integration between lipidomics and clinical phenomes in patients with acute lung infection, pulmonary embolism, or acute exacerbation of chronic pulmonary diseases: a preliminary study

Cited by 20 publications

References 29 publications

Trans‐omic profiling between clinical phenoms and lipidomes among patients with different subtypes of lung cancer

Trans‐omic profiling between clinical phenoms and lipidomes among patients with different subtypes of lung cancer

Advancing Semen Evaluation Using Lipidomics

Lipid Mediators in Critically Ill Patients: A Step Towards Precision Medicine

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