Agammaglobulinemia: causative mutations and their implications for novel therapies

Berglöf, Anna; Turunen, Janne; Gissberg, Olof; Bestas, Burcu; Blomberg, K. Emelie M.; Smith, C. I. Edvard

doi:10.1586/1744666x.2013.850030

Cited by 27 publications

(24 citation statements)

References 102 publications

(114 reference statements)

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“…A trend towards decrease in CD16 + SLAN + monocytes, which produce high levels of TNF‐α (Wong et al , ), was observed at day 29. To elucidate whether this was directly depending on BTK‐inhibition in monocytes, we measured SLAN expression on monocytes from a patient with XLA, a condition characterized by loss of functional BTK (Vetrie et al , ; Berglof et al , ). Indeed, we observed extremely few SLAN + monocytes (Figure S6), suggesting that their presence depends on BTK signalling and that the observed decrease in CD16 + SLAN + monocytes was related to ibrutinib treatment.…”

Section: Discussionmentioning

confidence: 99%

Ibrutinib induces rapid down‐regulation of inflammatory markers and altered transcription of chronic lymphocytic leukaemia‐related genes in blood and lymph nodes

et al. 2018

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In chronic lymphocytic leukaemia (CLL) patients, treatment with the Bruton tyrosine kinase inhibitor ibrutinib induces a rapid shift of tumour cells from lymph nodes (LN) to peripheral blood (PB). Here, we characterized in depth the dynamics of ibrutinib-induced inflammatory, transcriptional and cellular changes in different compartments immediately after treatment initiation in seven relapsed/refractory CLL patients. Serial PB and LN samples were taken before start and during the first 29 days of treatment. Changes in plasma inflammation-related biomarkers, CLL cell RNA expression, B-cell activation and migration markers expression, and PB mononuclear cell populations were assessed. A significant reduction of 10 plasma inflammation markers, the majority of which were chemokines and not CLL-derived, was observed within hours, and was paralleled by very early increase of CD19 circulating cells. At the RNA level, significant and continuous changes in transcription factors and signalling molecules linked to B-cell receptor signalling and CLL biology was observed in both PB and LN CLL cells already after 2 days of treatment. In conclusion, ibrutinib seems to instantly shut off an ongoing inflammatory response and interfere with diverse sensitive pathways in the LN.

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Section: Discussionmentioning

confidence: 99%

Ibrutinib induces rapid down‐regulation of inflammatory markers and altered transcription of chronic lymphocytic leukaemia‐related genes in blood and lymph nodes

et al. 2018

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“…The primary B lymphocytes responding to the vaccine would subsequently maturate into BTK-independent long-lived plasma cells exerting long-term protection. Due to the fact that the B cell receptor is not expressed in plasma cells, this strategy is valid for all primary immunodeficiencies caused by splice site mutations affecting this receptor complex (1).…”

Section: Discussionmentioning

confidence: 99%

“…X-linked agammaglobulinemia (XLA) is the most common form of inherited agammaglobulinemia, accounting for 85% of all cases (1,2). In this disease, a B cell lineage developmental block, manifested at the transition between the pro-B and pre-B cell stages (3), leads to the essential lack of mature B and plasma cells, with a concomitant pronounced reduction of immunoglobulin levels.…”

Section: Introductionmentioning

confidence: 99%

Splice-correcting oligonucleotides restore BTK function in X-linked agammaglobulinemia model

Bestas¹,

Moreno²,

Blomberg³

et al. 2014

J. Clin. Invest.

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“…BTK is a non-receptor tyrosine kinase that belongs to the TEC family kinases (TFK), which is the second largest family of non-receptor kinases in humans [3]. BTK is known to be an essential component of B cell receptor (BCR) signalling and is involved in B cell differentiation, proliferation and survival [4,5]. Many studies have reported an essential role of BCR signalling in the pathogenesis of several B cell malignancies [6].…”

Section: Introductionmentioning

confidence: 99%

Targets for Ibrutinib Beyond B Cell Malignancies

et al. 2015

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Ibrutinib (Imbruvica™) is an irreversible, potent inhibitor of Bruton's tyrosine kinase (BTK). Over the last few years, ibrutinib has developed from a promising drug candidate to being approved by FDA for the treatment of three B cell malignancies, a truly remarkable feat. Few, if any medicines are monospecific and ibrutinib is no exception; already during ibrutinib's initial characterization, it was found that it could bind also to other kinases. In this review, we discuss the implications of such interactions, which go beyond the selective effect on BTK in B cell malignancies. In certain cases, the outcome of ibrutinib treatment likely results from the combined inhibition of BTK and other kinases, causing additive or synergistic, effects. Conversely, there are also examples when the clinical outcome seems unrelated to inhibition of BTK. Thus, more specifically, adverse effects such as enhanced bleeding or arrhythmias could potentially be explained by different interactions. We also predict that during long‐term treatment bone homoeostasis might be affected due to the inhibition of osteoclasts. Moreover, the binding of ibrutinib to molecular targets other than BTK or effects on cells other than B cell‐derived malignancies could be beneficial and result in new indications for clinical applications.

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Agammaglobulinemia: causative mutations and their implications for novel therapies

Cited by 27 publications

References 102 publications

Ibrutinib induces rapid down‐regulation of inflammatory markers and altered transcription of chronic lymphocytic leukaemia‐related genes in blood and lymph nodes

Ibrutinib induces rapid down‐regulation of inflammatory markers and altered transcription of chronic lymphocytic leukaemia‐related genes in blood and lymph nodes

Splice-correcting oligonucleotides restore BTK function in X-linked agammaglobulinemia model

Targets for Ibrutinib Beyond B Cell Malignancies

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