Your search keyword '"Packham, Graham"' showing total 11 results

1. Targeted inhibition of eIF4A suppresses B-cell receptor-induced translation and expression of MYC and MCL1 in chronic lymphocytic leukemia cells.

Author

Wilmore, Sarah, Rogers-Broadway, Karly-Rai, Taylor, Joe, Lemm, Elizabeth, Fell, Rachel, Stevenson, Freda K., Forconi, Francesco, Steele, Andrew J., Coldwell, Mark, Packham, Graham, and Yeomans, Alison

Subjects

CHRONIC lymphocytic leukemia, B cell receptors, MYC proteins, B cells, PROTEIN expression

Abstract

Signaling via the B-cell receptor (BCR) is a key driver and therapeutic target in chronic lymphocytic leukemia (CLL). BCR stimulation of CLL cells induces expression of eIF4A, an initiation factor important for translation of multiple oncoproteins, and reduces expression of PDCD4, a natural inhibitor of eIF4A, suggesting that eIF4A may be a critical nexus controlling protein expression downstream of the BCR in these cells. We, therefore, investigated the effect of eIF4A inhibitors (eIF4Ai) on BCR-induced responses. We demonstrated that eIF4Ai (silvestrol and rocaglamide A) reduced anti-IgM-induced global mRNA translation in CLL cells and also inhibited accumulation of MYC and MCL1, key drivers of proliferation and survival, respectively, without effects on upstream signaling responses (ERK1/2 and AKT phosphorylation). Analysis of normal naïve and non-switched memory B cells, likely counterparts of the two main subsets of CLL, demonstrated that basal RNA translation was higher in memory B cells, but was similarly increased and susceptible to eIF4Ai-mediated inhibition in both. We probed the fate of MYC mRNA in eIF4Ai-treated CLL cells and found that eIF4Ai caused a profound accumulation of MYC mRNA in anti-IgM treated cells. This was mediated by MYC mRNA stabilization and was not observed for MCL1 mRNA. Following drug wash-out, MYC mRNA levels declined but without substantial MYC protein accumulation, indicating that stabilized MYC mRNA remained blocked from translation. In conclusion, BCR-induced regulation of eIF4A may be a critical signal-dependent nexus for therapeutic attack in CLL and other B-cell malignancies, especially those dependent on MYC and/or MCL1. [ABSTRACT FROM AUTHOR]

Published

2021

2. The role of the B-cell receptor in the pathogenesis of chronic lymphocytic leukaemia

Author

Packham, Graham and Stevenson, Freda

Subjects

*B cells, *CELL receptors, *CHRONIC lymphocytic leukemia, *CARCINOGENESIS, *IMMUNOGLOBULINS, *CELL differentiation, *HEALTH outcome assessment

Abstract

Abstract: The key molecule for normal B cells is the surface Ig (sIg) of the B-cell receptor, which influences cell behaviour, even after neoplastic transformation. During B-cell maturation, sIg accumulates somatic mutations in the Ig variable region (V) genes and tumours retain these patterns, thereby revealing the point of differentiation of the B cell of origin. The importance of origin is strikingly illustrated in CLL where the two major subsets with distinctive clinical behaviour express either unmutated (U) or mutated (M) V genes. Biased selection of VDJ genes also occurs in CLL, allowing further identification of the normal B-cell counterparts, with U-CLL apparently derived from circulating naïve B cells. Surface IgM of CLL is functional, with evidence for ongoing interaction with antigen in vivo. Signalling connects to cell survival, proliferation and migration, key determinants of tumour cell behaviour. Probing of B-cell receptor-mediated signalling pathways, either constitutively activated or open for activation, reveals dynamic, possibly repetitive, stimulatory events, likely to occur in tissue sites. Subtle differences in signal responsiveness between U-CLL or M-CLL subsets, together with microenvironmental factors, may explain clinical outcome. Knowledge of the critical signalling pathways should reveal the steps vulnerable to inhibition and allow development of a new range of therapeutic drugs, targeted particularly against the more aggressive subset, U-CLL. [ABSTRACT FROM AUTHOR]

Published

2010

3. DNA binding of USF is required for specific E-box dependent gene activation in vivo.

Author

Kiermaier, Astrid, Gawn, Jonathan M, Desbarats, Laurie, Saffrich, Rainer, Ansorge, Wilhelm, Farrell, Paul J, Eilers, Martin, and Packham, Graham

Subjects

MYC proteins, GENETIC regulation, B cells

Abstract

Although USF-1 and -2 are the major proteins that bind to Myc-regulated E-box (CACGTG) elements in many cells, there is no clear role for USF during Myc-dependent gene regulation. Using dominant negative alleles of USF-1 we now show that DNA binding by USF at a Myc-regulated E-box limits the ability of another E-box binding factor, TFE-3, to activate a target gene of Myc in vivo and to stimulate S phase entry in resting fibroblasts. Similarly, dominant negative alleles of USF-1 relieve the restriction that prevents activation of the IgH enhancer by TFE-3 in non B-cells. DNA binding activity of USF complexes is abundant in primary human B-cells and is significantly downregulated during B-cell immortalization. Re-expression of USF-1 in immortalized B-cells retards proliferation. Our data establish an essential role for USF in restricting E-box dependent gene activation in vivo and suggest that this control is relaxed during cellular immortalization. [ABSTRACT FROM AUTHOR]

Published

1999

4. Lectins from opportunistic bacteria interact with acquired variable-region glycans of surface immunoglobulin in follicular lymphoma.

Author

Schneider, Dunja, Dühren-von Minden, Marcus, Alkhatib, Alabbas, Setz, Corinna, van Bergen, Cornelis A. M., Benkißer-Petersen, Marco, Wilhelm, Isabel, Villringer, Sarah, Krysov, Sergey, Packham, Graham, Zirlik, Katja, Römer, Winfried, Buske, Christian, Stevenson, Freda K., Veelken, Hendrik, and Jumaa, Hassan

Subjects

*LECTINS, *GLYCANS, *LYMPHOMA treatment, *B cells, *ANTIGEN receptors, *AUTOANTIGENS, *IMMUNOGLOBULINS, *GLYCOSYLATION

Abstract

B-cell antigen receptor (BCR) expression is a key feature of most B-cell lymphomas, but the mechanisms of BCR signal induction and the involvement of autoantigen recognition remain unclear. In follicular lymphoma (FL) B cells, BCR expression is retained despite a chromosomal translocation that links the antiapoptotic gene BCL2 to the regulatory elements of immunoglobulin genes, thereby disrupting 1 heavy-chain allele. A remarkable feature of FL-BCRs is the acquisition of potential N-glycosylation sites during somatic hypermutation. The introduced glycans carry mannose termini, which create potential novel binding sites for mannose-specific lectins. Here, we investigated the effect of N-linked variable-region glycosylation for BCR interaction with cognate antigen and with lectins of different origins. N-glycans were found to severely impair BCR specificity and affinity to the initial cognate antigen. In addition, we found that lectins from Pseudomonas aeruginosa and Burkholderia cenocepacia bind and stimulate FL cells. Human exposure to these bacteria can occur by contact with soil and water. In addition, they represent opportunistic pathogens in susceptible hosts. Understanding the role of bacterial lectins might elucidate the pathogenesis of FL and establish novel therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published

2015

5. BTK-independent regulation of calcium signalling downstream of the B-cell receptor in malignant B-cells.

Author

Arthur, Rachael, Wathen, Alexander, Lemm, Elizabeth A., Stevenson, Freda K., Forconi, Francesco, Linley, Adam J., Steele, Andrew J., Packham, Graham, and Valle-Argos, Beatriz

Subjects

*LYMPHOCYTIC leukemia, *CHRONIC leukemia, *CALCIUM, *B cells, *INTRACELLULAR calcium, *BRUTON tyrosine kinase

Abstract

BTK inhibitors (BTKi) have dramatically improved outcomes for patients with chronic lymphocytic leukaemia (CLL) and some forms of B-cell lymphoma. However, new strategies are needed to enhance responses. Here we have performed a detailed analysis of the effects of BTKi on B-cell receptor (BCR)-induced signalling using primary malignant cells from CLL patients and B-lymphoma cell lines. Although BTK is considered as a key activator of PLCγ2, BTKi (ibrutinib and acalabrutinib) failed to fully inhibit calcium responses in CLL samples with strong BCR signalling capacity. This BTKi-resistant calcium signalling was sufficient to engage downstream calcium-dependent transcription and suppress CLL cell apoptosis and was entirely independent of BTK and not just its kinase activity as similar results were obtained using a BTK-degrading PROTAC. BTK-independent calcium signalling was also observed in two B-lymphoma cell lines where BTKi had little effect on the initial phase of the calcium response but did accelerate the subsequent decline in intracellular calcium. In contrast to BTKi, calcium responses were completely blocked by inhibition of SYK in CLL and lymphoma cells. Engagement of BTK-independent calcium responses was associated with BTK-independent phosphorylation of PLCγ2 on Y753 and Y759 in both CLL and lymphoma cells. Moreover, in CLL samples, inhibition of RAC, which can mediate BTK-independent activation of PLCγ2, cooperated with ibrutinib to suppress calcium responses. BTK-independent calcium signalling may limit the effectiveness of BTKi to suppress BCR signalling responses and our results suggest inhibition of SYK or dual inhibition of BTK and RAC as alternative strategies to strengthen pathway blockade. • Efficacy of BTKi against BCR-induced Ca2+ responses varies between CLL samples • BTK-independent signals can promote CLL cell survival and transcriptional responses • BTK-independent Ca2+ responses are associated with retained PLCγ2 phosphorylation • RAC inhibition and ibrutinib cooperate to suppress Ca2+ responses in CLL cells [ABSTRACT FROM AUTHOR]

Published

2022

6. B-cell receptor signaling induces proteasomal degradation of PDCD4 via MEK1/2 and mTORC1 in malignant B cells.

Author

Taylor, Joe, Wilmore, Sarah, Marriot, Sophie, Rogers-Broadway, Karly-Rai, Fell, Rachel, Minton, Annabel R., Branch, Tom, Ashton-Key, Meg, Coldwell, Mark, Stevenson, Freda K., Forconi, Francesco, Steele, Andrew J., Packham, Graham, and Yeomans, Alison

Subjects

*CANCER cells, *CHRONIC lymphocytic leukemia, *B cells, *MYC proteins, *RNA regulation, *CD19 antigen, *MESSENGER RNA, *PROTEASOME inhibitors

Abstract

B-cell receptor (BCR) signaling plays a major role in the pathogenesis of B-cell malignancies and is an established target for therapy, including in chronic lymphocytic leukemia cells (CLL), the most common B-cell malignancy. We previously demonstrated that activation of BCR signaling in primary CLL cells downregulated expression of PDCD4, an inhibitor of the translational initiation factor eIF4A and a potential tumor suppressor in lymphoma. Regulation of the PDCD4/eIF4A axis appeared to be important for expression of the MYC oncoprotein as MYC mRNA translation was increased following BCR stimulation and MYC protein induction was repressed by pharmacological inhibition of eIF4A. Here we show that MYC expression is also associated with PDCD4 down-regulation in CLL cells in vivo and characterize the signaling pathways that mediate BCR-induced PDCD4 down-regulation in CLL and lymphoma cells. PDCD4 downregulation was mediated by proteasomal degradation as it was inhibited by proteasome inhibitors in both primary CLL cells and B-lymphoma cell lines. In lymphoma cells, PDCD4 degradation was predominantly dependent on signaling via the AKT pathway. By contrast, in CLL cells, both ERK and AKT pathways contributed to PDCD4 down-regulation and dual inhibition using ibrutinib with either MEK1/2 or mTORC1 inhibition was required to fully reverse PDCD4 down-regulation. Consistent with this, dual inhibition of BTK with MEK1/2 or mTORC1 resulted in the strongest inhibition of BCR-induced MYC expression. This study provides important new insight into the regulation of mRNA translation in B-cell malignancies and a rationale for combinations of kinase inhibitors to target translation control and MYC expression. • B-cell receptor signaling induces rapid PDCD4 downregulation in malignant B cells. • PDCD4 downregulation is dependent on increased proteasomal degradation. • PDCD4 downregulation is mediated via the mTORC1/p70-S6K and ERK1/2 pathways. • PDCD4 downregulation correlates with increased MYC expression in vitro and in vivo. [ABSTRACT FROM AUTHOR]

Published

2022

7. Variable induction of PRDM1 and differentiation in chronic lymphocytic leukemia is associated with anergy.

Author

Duckworth, Andrew, Glenn, Mark, Slupsky, Joseph R., Packham, Graham, and Kalakonda, Nagesh

Subjects

*B cells, *CHRONIC lymphocytic leukemia, *CELL differentiation, *NUCLEOTIDES, *CELL proliferation, *APOPTOSIS

Abstract

Despite antigen engagement and intact B-cell-receptor (BCR) signaling, chronic lymphocytic leukemia (CLL) cells fail to undergo terminal differentiation. We hypothesized that such failure may be due to anergy, as CLL cells exhibit variable levels of nonresponsiveness to surface IgM stimulation that is reversible in vitro. Moreover, anergy is associated with reduced differentiation capacity in normal B cells. We investigated responses of CLL cells to two potent differentiation-promoting agents, IL-21 and cytosine guanine dinucleotide-enriched oligo-deoxynucleotides. The induction of PR domain-containing protein 1 (PRDM1; also known as Blimp-1), a critical regulator of plasmacytic differentiation, by these agents was closely correlated but varied between individual cases, despite functionally intact iL-21 receptor- and Toll-like receptor 9-mediated signal transducer and activator of transcription 3, and nuclear factor-KB pathways. PRDM1 induction was inversely correlated with the extent of anergy as measured by the ability to mobilize intracellular Ca2+ following BCR crosslinking. PRDM1 responsiveness was associated with other markers of differentiation and proliferation but not with differences in apoptosis. The ability to induce PRDM1 did correlate with differential transcriptional and epigenetic regulation of the PRDM1 gene. These studies extend our understanding of CLL pathobiology, demonstrating that reduced differentiation capacity may be a consequence of anergy. Epigenetic drugs may offer possibilities to reactivate PRDM1 expression as part of novel differentiation therapy approaches. [ABSTRACT FROM AUTHOR]

Published

2014

8. The IGHV1-69/IGHJ3 recombinations of unmutated CLL are distinct from those of normal B cells.

Author

Forconi, Francesco, Potter, Kathleen N., Sozzi, Elisa, Henderson, Isla, Cencini, Emanuele, Rossi, Davide, Bomben, Riccardo, Gattei, Valter, Gaidano, Gianluca, Packham, Graham, and Stevenson, Freda K.

Subjects

*B cells, *GENE expression, *CHRONIC lymphocytic leukemia, *STEREOTYPES, *AMINO acids, *HOMOLOGY (Biology), *GENE rearrangement

Abstract

IGHV1-69/51p1 is expressed by ∼ 30% of unmutated chronic lymphocytic leukemia (U-CLL) and combines with selected IGHD and 1GHJ genes generating stereotypes if HCDR3 amino acid homology is > 60%. We had previously revealed stereotypic IGHV1-69/IGHJ6 rearrangements in normal naive B cells, thereby identifying potential counterparts of U-CLL. A different stereotypic IGHV1-69/IGHD3-16(RF2)/IGHJ3 rearrangement carrying the CAR(GGx)YD motif in the N1-region, recurrent in 6% IGHV1-69+ve CLL, is exceptionally sequence restricted, strongly suggestive of shared antigen recognition. We have now analyzed 1GHV1-69/1GHJ3 rearrangements in circulating B cells of healthy individuals using several PCR-based approaches with IGHV1-69/IGHJ3 CLL sequences for reference. Stereotypes were found, but all were distinct from CLL. Remarkably, even a highly sensitive semi-nested PCR, specific for the CLL-expressed IGHV1-69/IGHD3-16(RF2)/ IGHJ3 stereotype, failed to identify the CAR(GGx)YD sequence, although similar motifs were found. These highly specific B cells are not apparent in the accessible normal repertoire and may expand in response to rarely expressed antigens important in the pathogenesis of CLL [ABSTRACT FROM AUTHOR]

Published

2012

9. Mechanisms and clinical significance of BIM phosphorylation in chronic lymphocytic leukemia.

Author

Paterson, Alex, Mockridge, C. Ian, Adams, Jemimah E., Krysov, Sergey, Potter, Kathleen N., Duncombe, Andrew S., Cook, Simon J., Stevenson, Freda K., and Packham, Graham

Subjects

*B cells, *PHOSPHORYLATION, *CHRONIC lymphocytic leukemia diagnosis, *APOPTOSIS, *KINASES

Abstract

B-cell receptor and microenvironment-derived signals promote accumulation of chronic lymphocytic leukemia (CLL) cells through increased proliferation and/or decreased apoptosis. In this study, we Investigated the regulation of BIM, a proapoptotic BCL2-related protein, which is tightly regulated by phosphorylation. Surface 1gM stimulation increased phosphorylation of 2 BIM isoforms, BIMEL and BIML, in a subset of CLL samples. In contrast, in normal B cells, anti-lgM triggered selective phosphorylation of BIMEL only. In CLL, anti-lgM-induced BIM phosphorylation correlated with unmutated IGHVgene status and with progressive disease. Strikingly, it was also associated with progressive disease within the mutated IGHV gene subset. BIM phosphorylation was dependent on MEK1/2 kinase activity, and we identified BIMEL serine 69, previously linked to pro-survival responses, as the major site of phosphorylation in CLL and in Ramos cells. BIMEL/BIML phosphorylation was associated with release of the pro-survival protein MCL1. Coculture of CLL cells with HK cells, a model of the CLL microenvironment, promoted CLL cell survival and was associated with MEK1I2 activation and BIMEL phosphorylation. Hence, BIM phosphorylation appears to play a key role in apoptosis regulation in CLL cells, potentially coordinating antigen and microenvironmentderived survival signals. Antigenmediated effects on BIM may be an important determinant of clinical behavior. [ABSTRACT FROM AUTHOR]

Published

2012

10. B-cell receptor signaling in chronic lymphocytic leukemia.

Author

Stevenson, Freda K., Krysov, Sergey, Davies, Andrew J., Steele, Andrew J., and Packham, Graham

Subjects

*B cells, *CELL receptors, *CHRONIC lymphocytic leukemia, *RECOMBINANT blood proteins, *GENETIC mutation, *ANTIGENS, *BLOOD cells

Abstract

The B-cell receptor (8CR) is a key survival molecule for normal B cells and for most B-cell malignancies. Recombinatorial and mutational patterns in the clonal lmmunoglobulin (Ig) of chronic lymphocytic leukemia (CLL) have revealed 2 major lgMD-expressing subsets and an isotype-switched variant, each developing from distinct B-cell populations. Tracking of conserved stereotypic features of Ig variable regions characteristic of U.CLL indicate circulating naive B cells as the likely cells of origin. in CLL, engagement of the 8CR by antigen occurs in vivo, leading to down-regulated expression and to an unanticipated modulation of glycosylation of surface 1gM, visible in blood cells, especially in U-CLL. Modulated giycofornis of slgM are signal competent and could bind to environmental lectins. U-CLL cases express more slgM and have Increased signal competence, linking differential signaling responses to clinical behavior. Mapping of 8CR signaling pathways identifies targets for blockade, aimed to deprive CLL cells of survival and proliferative signals New inhibitors of BCR signaling appear to have clinical activity. in this Perspective, we discuss the functIonal significance of the 8CR in CLL, and we describe strategies to target BCR signaling as an emerging therapeutic approach. [ABSTRACT FROM AUTHOR]

Published

2011

11. Induction of Cytosolic Calcium Flux by CD20 Is Dependent upon B Cell Antigen Receptor Signaling.

Author

Walshe, Claire A., Beers, Stephen A., French, Ruth R., Chan, Claude H. T., Johnson, Peter W., Packham, Graham K., Glennie, Martin J., and Cragg, Mark S.

Subjects

*B cells, *ANTIGENS, *CELL receptors, *HODGKIN'S disease, *MONOCLONAL antibodies

Abstract

The anti-CD20 monoclonal antibody (mAb) rituximab is now routinely used for the treatment of non-Hodgkins lymphoma and is being examined in a wide range of other B-cell disorders, such as rheumatoid arthritis. Despite intensive study, the mechanism of action still remains uncertain. In the current study, anti-CD20 mAb-induced calcium signaling was investigated. Previously, we grouped anti-CD20 mAbs into Type I (rituximab-like) and Type II (BI-like) based upon various characteristics such as their ability to induce complement activation and redistribute CD20 into detergent-insoluble membrane domains. Here we show that only Type I mAbs are capable of inducing a calcium flux in B cells and that this is tightly correlated with the expression of the B-cell antigen receptor (BCR). Inhibitor analysis revealed that the signaling cascade employed by CD20 was strikingly similar to that utilized by the BCR, with inhibitors of Syk, Src, and PI3K, but not EGTA, p38, or ERK1/2, completely ablating calcium flux. Furthermore, binding of Type I but not Type II mAbs caused direct association of CD20 with the BCR as measured by FRET and resulted in the phosphorylation of BCR-specific adaptor proteins BLNK and SLP-76. Crucially, variant Ramos cells lacking BCR expression but with unchanged CD20 expression were completely unable to induce calcium flux following ligation of CD20. Collectively, these data indicate that CD20 induces cytosolic calcium flux through its ability to associate with and "hijack" the signaling potential of the BCR. [ABSTRACT FROM AUTHOR]

Published

2008