Serum N‐glycan analysis in breast cancer patients – Relation to tumour biology and clinical outcome

Haakensen, Vilde Drageset; Steinfeld, Israel; Saldova, Radka; Shehni, Akram Asadi; Kifer, Ilona; Naume, Bjørn; Rudd, Pauline M.; Børresen-Dale, Anne Lise; Yakhini, Zohar

doi:10.1016/j.molonc.2015.08.002

Cited by 35 publications

(32 citation statements)

References 46 publications

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“…Haakensen et al . () observed that this glycan is correlated with decreased mitochondrial fatty acid beta oxidation. Decrease in this glycan in cancer indicates an increase in cell energy production.…”

Section: Discussionmentioning

confidence: 91%

“…All glycans and derived glycan features were assigned in Saldova et al (2014). The major glycans in each peak, selected in Haakensen et al (2016), are summarized in Table 2.…”

Section: Resultsmentioning

confidence: 99%

“…, Table ). In previous studies, we have found that it strongly correlates with increased BMI and is associated with decreased integrin‐mediated cell adhesion and decreased adipocyte activity (Haakensen et al ., ). An increase in BMI reduces adipocyte activity and increases inflammation and the risk of cancer (van Kruijsdijk et al ., ).…”

Section: Discussionmentioning

confidence: 97%

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Serum N‐glycome alterations in breast cancer during multimodal treatment and follow‐up

et al. 2017

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Using our recently developed high‐throughput automated platform, N‐glycans from all serum glycoproteins from patients with breast cancer were analysed at diagnosis, after neoadjuvant chemotherapy, surgery, radiotherapy and up to 3 years after surgery. Surprisingly, alterations in the serum N‐glycome after chemotherapy were pro‐inflammatory with an increase in glycan structures associated with cancer. Surgery, on the other hand, induced anti‐inflammatory changes in the serum N‐glycome, towards a noncancerous phenotype. At the time of first follow‐up, glycosylation in patients with affected lymph nodes changed towards a malignant phenotype. C‐reactive protein showed a different pattern, increasing after first line of neoadjuvant chemotherapy, then decreasing throughout treatment until 1 year after surgery. This may reflect a switch from acute to chronic inflammation, where chronic inflammation is reflected in the serum after the acute phase response subsides. In conclusion, we here present the first time‐course serum N‐glycome profiling of patients with breast cancer during and after treatment. We identify significant glycosylation changes with chemotherapy, surgery and follow‐up, reflecting the host response to therapy and tumour removal.

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Section: Discussionmentioning

confidence: 91%

“…All glycans and derived glycan features were assigned in Saldova et al (2014). The major glycans in each peak, selected in Haakensen et al (2016), are summarized in Table 2.…”

Section: Resultsmentioning

confidence: 99%

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Serum N‐glycome alterations in breast cancer during multimodal treatment and follow‐up

et al. 2017

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“…After separation by hydrophilic‐interaction chromatography (HILIC) or capillary electrophoresis, glycans are identified by mass spectrometry . Identification of individual oligosaccharides by their retention time in HILIC, enables very fast analysis of glycome, especially in biological fluids such as serum plasma, or urine . Profiling of both cell‐surface and intracellular glycans is more complicated and requires additional steps such as cell or tissue homogenization and fractionation .…”

Section: Analytical Approachesmentioning

confidence: 99%

“… underlined the necessity for a “multi‐omics” approach and data analysis in order to understand “the transition from healthy physiology to a disease state.” Haakensen et al. used this approach, and by studying the serum glycome and tumor transcriptome (mRNA and miRNA), they could demonstrate that the presence of circulating tumor cells is associated with certain glycome structures. Recent reviews present this approach, and its possible use for the optimization of different cancer therapies is widely discussed .…”

Section: Analytical Approachesmentioning

confidence: 99%

Glycosylation and metastases

2018

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The change of cellular glycosylation is one of the key events in malignant transformation and neoplastic progression, and tumor‐related glycosylation alterations are promising targets in both tumor diagnosis and therapy. Both malignant transformation and neoplastic progression are the consequence of gene expression alterations and alterations in protein expression. Micro environmental factors such as extracellular matrix (ECM) also play an important role in their growth and metastasis. Tumor‐associated glycans are important biomarker candidates for cancer diagnosis and prognosis, and analytical methods for their detection were developed recently. Glycoproteomics that use mass spectrometry for identification of cancer antigens and structural analysis of glycans play a key role in the investigation of changes of glycosylation during malignant transformation and tumor development and metastasis. Deep understanding of glycan remodeling in cancer and the role of glycosyltransferases that are involved in this process will require a detailed profiling of glycosylation patterns of tumor cells, and corresponding analytical methods for their detection were developed.

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Lectin Affinity Chromatography for the Discovery of Novel Cancer Glycobiomarkers: A Case Study with PSA Glycoforms and Prostate Cancer

Llop

Peracaula

2021

Methods in Molecular Biology

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Serum N‐glycan analysis in breast cancer patients – Relation to tumour biology and clinical outcome

Cited by 35 publications

References 46 publications

Serum N‐glycome alterations in breast cancer during multimodal treatment and follow‐up

Serum N‐glycome alterations in breast cancer during multimodal treatment and follow‐up

Glycosylation and metastases

Lectin Affinity Chromatography for the Discovery of Novel Cancer Glycobiomarkers: A Case Study with PSA Glycoforms and Prostate Cancer

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