Proteomics and metabolomics identify molecular mechanisms of aging potentially predisposing for chronic lymphocytic leukemia

Mayer, Rupert L.; Schwarzmeier, Josef D.; Gerner, Marlene C.; Bileck, Andrea; Mader, Johanna C.; Meier‐Menches, Samuel M.; Gerner, Samuel M.; Schmetterer, Klaus G.; Pukrop, Tobias; Reichle, Albrecht; Slany, Astrid; Gerner, Christopher

doi:10.1074/mcp.ra117.000425

Cited by 48 publications

(65 citation statements)

References 94 publications

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“…MIF secretion is robustly induced by oxidative stress (Gupta et al , ), which is supported by our data showing that CLL cells have higher expression of several antioxidant species (e.g. TXNRD2, GSTP1, SOD1, TXN) and evidence from the literature showing that CLL cells have high levels of intracellular ROS species (Mayer et al , ). Low levels of PNP have also been previously reported in CLL (Huang et al , ).…”

Section: Resultssupporting

confidence: 87%

“…The availability of mass spectrometry (MS) late last century led to studies investigating the CLL proteome. These analyses identified a limited number of differentially expressed proteins not only between M-and UM-CLL (Cochran et al, 2003;Barnidge et al, 2005;Scielzo et al, 2005;Rees-Unwin et al, 2010;Alsagaby et al, 2014;Eagle et al, 2015), but also between healthy B cells and B-CLL cells (Johnston et al, 2018;Mayer et al, et al 2018). This is most likely not an accurate representation of the true proteomic differences between these cell types, given their vastly divergent lifespans and functions in the body.…”

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confidence: 99%

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Altered expression of metabolic pathways in CLL detected by unlabelled quantitative mass spectrometry analysis

et al. 2019

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Summary Chronic lymphocytic leukaemia (CLL) remains the most common incurable malignancy of B cells in the western world. Patient outcomes are heterogeneous and can be difficult to predict with current prognostic markers. Here, we used a quantitative label‐free proteomic technique to ascertain differences in the B‐cell proteome from healthy donors and CLL patients with either mutated (M‐CLL) or unmutated (UM‐CLL) IGHV to identify new prognostic markers. In peripheral B‐CLL cells, 349 (22%) proteins were differentially expressed between normal B cells and B‐CLL cells and 189 (12%) were differentially expressed between M‐CLL and UM‐CLL. We also examined the proteome of proliferating CLL cells in the lymph nodes, and identified 76 (~8%) differentially expressed proteins between healthy and CLL lymph nodes. B‐CLL cells show over‐expression of proteins involved in lipid and cholesterol metabolism. A comprehensive lipidomic analysis highlighted large differences in glycolipids and sphingolipids. A shift was observed from the pro‐apoptotic lipid ceramide towards the anti‐apoptotic/chemoresistant lipid, glucosylceramide, which was more evident in patients with aggressive disease (UM‐CLL). This study details a novel quantitative proteomic technique applied for the first time to primary patient samples in CLL and highlights that primary CLL lymphocytes display markers of a metabolic shift towards lipid synthesis and breakdown.

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Section: Resultssupporting

confidence: 87%

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confidence: 99%

Altered expression of metabolic pathways in CLL detected by unlabelled quantitative mass spectrometry analysis

et al. 2019

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“…This study identified both proteins as NOS2‐dependent synapto‐SNO proteins that increased during aging in APP/PS1 mice. NDUFAB1 regulation was previously related to aging and has been shown to be responsible for oxidative phosphorylation and down‐regulated in AD patients (Kim et al ; Mayer et al ; Akila Parvathy Dharshini et al ). NDUFAB1 reduction may lead to energy metabolism impairment and result in neuronal cell death by apoptosis (Kim et al ).…”

Section: Discussionmentioning

confidence: 99%

Quantitative proteomics of synaptosome S‐nitrosylation in Alzheimer’s disease

Wijasa

Sylvester

Brocke‐Ahmadinejad

et al. 2019

Journal of Neurochemistry

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Increasing evidence suggests that both synaptic loss and neuroinflammation constitute early pathologic hallmarks of Alzheimer’s disease. A downstream event during inflammatory activation of microglia and astrocytes is the induction of nitric oxide synthase type 2, resulting in an increased release of nitric oxide and the post‐translational S‐nitrosylation of protein cysteine residues. Both early events, inflammation and synaptic dysfunction, could be connected if this excess nitrosylation occurs on synaptic proteins. In the long term, such changes could provide new insight into patho‐mechanisms as well as biomarker candidates from the early stages of disease progression. This study investigated S‐nitrosylation in synaptosomal proteins isolated from APP/PS1 model mice in comparison to wild type and NOS2−/− mice, as well as human control, mild cognitive impairment and Alzheimer’s disease brain tissues. Proteomics data were obtained using an established protocol utilizing an isobaric mass tag method, followed by nanocapillary high performance liquid chromatography tandem mass spectrometry. Statistical analysis identified the S‐nitrosylation sites most likely derived from an increase in nitric oxide (NO) in dependence of presence of AD pathology, age and the key enzyme NOS2. The resulting list of candidate proteins is discussed considering function, previous findings in the context of neurodegeneration, and the potential for further validation studies.

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“…19 Further evidence supporting dysregulated glutaminolysis was found in accompanying proteomic experiments which revealed increased levels of glutaminase and glutamine synthetase in CLL cells. 19 In comparison to normal lymphocytes, CLL cells have a dysregulated cell growth cycle and are primed for hypoxic response by constitutive low level expression of HIF-1α 20 even in normoxic environments such as circulating blood. Transcriptlevel expression of HIF-1α is variable among CLL patients 21 and has been correlated to unfavorable prognoses in a study of 88 CLL patients.…”

Section: Chronic Lymphocytic Leukemiamentioning

confidence: 90%

“…A mass spectrometry‐based metabolomic study of B lymphocytes from CLL patients (n = 4) in comparison to healthy controls (n = 5) revealed alterations in glutaminolysis in B‐CLL cells, specifically decreased levels of glutamine and glutamate and increased alanine, a product of glutaminolysis (Figure A) . Further evidence supporting dysregulated glutaminolysis was found in accompanying proteomic experiments which revealed increased levels of glutaminase and glutamine synthetase in CLL cells . In comparison to normal lymphocytes, CLL cells have a dysregulated cell growth cycle and are primed for hypoxic response by constitutive low level expression of HIF‐1α even in normoxic environments such as circulating blood.…”

Section: Chronic Lymphocytic Leukemiamentioning

confidence: 99%

Metabolic underpinnings of leukemia pathology and treatment

2018

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Background Carcinogenic transformation of white blood cells during hematopoiesis leads to the development of leukemia, a cancer characterized by incompetent immune cells and a disruption of normal bone marrow function. Leukemias are diverse in type, affected population, prognosis, and treatment regimen, yet a common theme in leukemia is the dysregulated metabolism of leukemic cells and leukemic stem cells with respect to their noncancerous counterparts. Recent findings In this review, we highlight current findings that elucidate metabolic traits unique to the four major types of leukemia, which confer carcinogenic survival but can be potentially exploited for therapeutic intervention. These metabolic features can work in conjunction with or be independent of unique aspects of the bone marrow microenvironment that can also influence cell survival and proliferation, thus sustaining carcinogenesis. Conclusion Deepening our understanding of the interactions of leukemias with their niche environments in vivo will inform future treatments for leukemia, particularly for those that are refractive to tyrosine kinase inhibitors and other therapeutic mainstays.

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Proteomics and metabolomics identify molecular mechanisms of aging potentially predisposing for chronic lymphocytic leukemia

Cited by 48 publications

References 94 publications

Altered expression of metabolic pathways in CLL detected by unlabelled quantitative mass spectrometry analysis

Altered expression of metabolic pathways in CLL detected by unlabelled quantitative mass spectrometry analysis

Quantitative proteomics of synaptosome S‐nitrosylation in Alzheimer’s disease

Metabolic underpinnings of leukemia pathology and treatment

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