Differential Induction of Apoptosis by Fludarabine Monophosphate in Leukemic B and Normal T Cells in Chronic Lymphocytic Leukemia

Consoli, Ugo; Eltounsi, Iman; Sandoval, Alex; Snell, Virginia; Kleine, Hans‐Dieter; Brown, Wendy; Robinson, Johnnie R.; DiRaimondo, Francesco; Plunkett, William; Andreeff, Michael

doi:10.1182/blood.v91.5.1742.1742_1742_1748

Cited by 12 publications

(16 citation statements)

References 22 publications

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“…As one of the major mechanisms of action of fludarabine is thought to be induction of apoptosis (Huang & Plunkett, 1995; Adkins et al , 1997; Bellosillo et al , 1997; Consoli et al , 1998; Kitada et al , 1998; Pettitt et al , 1999), we next verified whether fludarabine on its own could trigger the apoptotic cascade in Karpas 422 cells. Apoptosis was measured at different times by monoparametric Annexin V or biparametric TUNEL/DNA assay, using FACS analysis.…”

Section: Resultsmentioning

confidence: 86%

“…The molecular basis for the resistance or sensitivity to fludarabine‐induced apoptosis was investigated by analysing the expression of several molecules previously implicated in this process in Western blots, in particular fas, bcl‐2 and p53 (Fisher, 1994; Adkins et al , 1997; Bellosillo et al , 1997; Consoli et al , 1998; Kitada et al , 1998; Pettitt et al , 1999). No significant changes in levels of expression of these molecules was observed up to 48 h after fludarabine treatment in any of the cell lines and no correlation could be observed between expression levels and sensitivity to fludarabine‐induced apoptosis (data not shown).…”

Section: Discussionmentioning

confidence: 99%

“…Present evidence suggests that it acts through inhibition of DNA synthesis after incorporation of the active metabolite into DNA during replication and through inhibition of ribonucleotide reductase, DNA primase and DNA ligase (Plunkett et al , 1993; Adkins et al , 1997). Furthermore, evidence suggests that induction of apoptosis is an important mechanism of action of fludarabine (Huang & Plunkett, 1995; Adkins et al , 1997; Bellosillo et al , 1997; Consoli et al , 1998; Kitada et al , 1998; Pettitt et al , 1999). Our data show that different cell lines can show quite varied response to the same chemotherapeutic agent, as all four showed inhibition of cell growth, two (BJAB and WSU‐NHL) were induced into apoptosis and only one showed a strong response at RNA levels (Karpas 422).…”

Section: Discussionmentioning

confidence: 99%

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Synergism between fludarabine and rituximab revealed in a follicular lymphoma cell line resistant to the cytotoxic activity of either drug alone

Gaetano¹,

Xiao²,

Erba

et al. 2001

Br J Haematol

185

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Summary. We have shown previously that the anti-CD20 chimaeric monoclonal antibody rituximab exerts its effects on neoplastic B-lymphoma cell lines in part via complement-dependent cytotoxicity. In addition, membrane expression levels of complement inhibitory proteins CD55 and CD59 play a role in determining susceptibility to lysis. We have identified one t(14;18)-positive human B-cell non Hodgkin's lymphoma cell line (Karpas 422) that is resistant to rituximab and complement and used it for subsequent studies on the possible interaction between this novel therapeutic agent and established antineoplastic drugs. We have exposed Karpas to several chemotherapeutic agents (doxorubicin, idarubicin, cisplatin, taxol) for different time periods and subsequently exposed the cells to rituximab and human complement. The combination of these drugs with rituximab induced an additive cytotoxic effect. In contrast, exposure to fludarabine (1 mg/ml for 48±72 h) showed a synergistic effect, with cell lysis increasing from 10% to 20% using fludarabine or rituximab and complement alone to about 70% with both cytotoxic agents. Analysis of the mechanism for this synergistic effect showed that fludarabine downmodulates the membrane expression of CD55 (from 96% to 55% positive cells) without significantly altering CD20 levels. Northern analysis demonstrated that fludarabine induced a general downmodulation of steady state mRNA levels with no change in transcription rate detected in run-off assays. The study of the effect of fludarabine and rituximab in six freshly isolated B-cell chronic lymphocytic leukaemia (B-CLL) samples showed that, in most cases, fludarabine has an additive cytotoxic activity with rituximab and complement. This report gives a rational support for clinical studies with combinations of drugs, including monoclonal antibodies and fludarabine.

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Section: Resultsmentioning

confidence: 86%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Synergism between fludarabine and rituximab revealed in a follicular lymphoma cell line resistant to the cytotoxic activity of either drug alone

Gaetano¹,

Xiao²,

Erba

et al. 2001

Br J Haematol

185

View full text Add to dashboard Cite

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“…PNU156804 blocks IL-2dependent NF-kB and AP-1 activation [91] and it is a selective inhibitor of Janus tyrosine kinase 3(Jak3) [111] . Current B-CLL therapies do not demonstrate specificity, thus fludarabine is cytotoxic for T lymphocytes [109,110] . Interestingly, in a subset of samples, prodigiosin is less toxic than fludarabine for normal T cells, while having similar effect in B-CLL cells.…”

Section: Drawbacksmentioning

confidence: 99%

Review of Prodigiosin, Pigmentation in Serratia marcescens

Khanafari¹,

Assadi²,

Fakhr,³

2006

OnLine J. of Biological Sciences

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Prodigiosins, a family of natural red pigments characterized by a common pyrrolylpyrromethane skeleton, are produced by various bacteria that first characterized from Serratia marcescens. This pigment is a promising drug owing to its reported characteristics of having antifungal, immunosuppressive and anti-proliferative activity. From an industrial point of view to obtain optimal conditions to enhance the growth of Serratia marcescens and the pigment production is necessity. In present study, the production condition, physicochemical and functional characteristics, structure, genetic and gene expression, apoptosis and toxigenic effects of prodigiosin will be discussed in-order to contribute to the world of Serratia marcescens with respect to its prodigiosin production property

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“…Subsequently, intracellular phosphorylation takes place to the active metabolite fludarabine triphosphate (F-ara-ATP), which is built into the DNA and RNA, thereby inhibiting DNA/RNA synthesis. This leads to apoptosis in both chronic lymphocytic leukemia cells [ 5 ] and (with different susceptibility) in cell types targeted in the HCT setting [ 6 , 7 ].…”

Section: Introductionmentioning

confidence: 99%

Population Pharmacokinetics of Fludarabine in Children and Adults during Conditioning Prior to Allogeneic Hematopoietic Cell Transplantation

et al. 2018

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Background Fludarabine is often used as an important drug in reduced toxicity conditioning regimens prior to hematopoietic cell transplantation (HCT). As no definitive pharmacokinetic (PK) basis for HCT dosing for the wide age and weight range in HCT is available, linear body surface area (BSA)-based dosing is still used. Objective We sought to describe the population PK of fludarabine in HCT recipients of all ages. Methods From 258 HCT recipients aged 0.3–74 years, 2605 samples were acquired on days 1 (42%), 2 (17%), 3 (4%) and 4 (37%) of conditioning. Herein, the circulating metabolite of fludarabine was quantified, and derived concentration-time data were used to build a population PK model using non-linear mixed-effects modelling. Results Variability was extensive where area under the curve ranged from 10 to 66 mg h/L. A three-compartment model with first-order kinetics best described the data. Actual body weight (BW) with standard allometric scaling was found to be the best body-size descriptor for all PK parameters. Estimated glomerular filtration rate (eGFR) was included as a descriptor of renal function. Thus, clearance was differentiated into a non-renal (3.24 ± 20% L/h/70 kg) and renal (eGFR × 0.782 ± 11% L/h/70 kg) component. The typical volumes of distribution of the central (V1), peripheral (V2), and second peripheral (V3) compartments were 39 ± 8%, 20 ± 11%, and 50 ± 9% L/70 kg respectively. Intercompartmental clearances between V1 and V2, and V1 and V3, were 8.6 ± 8% and 3.8 ± 13% L/h/70 kg, respectively. Conclusion BW and eGFR are important predictors of fludarabine PK. Therefore, current linear BSA-based dosing leads to highly variable exposure, which may lead to variable treatment outcome.

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Differential Induction of Apoptosis by Fludarabine Monophosphate in Leukemic B and Normal T Cells in Chronic Lymphocytic Leukemia

Cited by 12 publications

References 22 publications

Synergism between fludarabine and rituximab revealed in a follicular lymphoma cell line resistant to the cytotoxic activity of either drug alone

Synergism between fludarabine and rituximab revealed in a follicular lymphoma cell line resistant to the cytotoxic activity of either drug alone

Review of Prodigiosin, Pigmentation in Serratia marcescens

Population Pharmacokinetics of Fludarabine in Children and Adults during Conditioning Prior to Allogeneic Hematopoietic Cell Transplantation

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