Interferon-α therapy in bcr-abl-negative myeloproliferative neoplasms

Kiladjian, Jean‐Jacques; Chomienne, Christine; Fenaux, Pierre

doi:10.1038/leu.2008.280

Cited by 152 publications

(140 citation statements)

References 93 publications

(84 reference statements)

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“…The median spleen sizes in centimeters below the left costal margin were 7.0 cm (range 0.0-24.0 cm) before treatment, and 0 cm (range 0.0-20.0 cm) at last follow-up (Table 1). Our results are thus in sharp contrast with those reported in the literature by Kiladjian et al 1 Bone marrow follow-up studies were possible in nine of the 13 patients, and were carried out a median of 2.3 years after the start of the rIFNa-2b therapy (range 1.2-5.0 years). The median duration of interferon treatment was 3.0 years (range 0.17-13.4 years).…”

contrasting

confidence: 56%

“…The use of interferon is based on its effects on megakaryopoiesis, which include decreasing megakaryocyte density and size, 2 inhibiting thrombopoietin-induced signaling, 3 suppressing the expression of transcription factors 4 and reducing levels of platelet-derived growth factor, 5 all of which play a major role in the pathogenesis of myelofibrosis. 1 The diagnosis of PM was established clinically, hematologically and by bone-marrow trephine biopsy, consistent with published criteria. [4][5][6] Pretreatment evaluation included history, physical examination, complete blood cell count and differential CD34 count, BCR-ABL and JAK2 V617F allele burden determinations, serum chemistries and thyroid function tests.…”

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confidence: 99%

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Recombinant interferon alpha (rIFNα-2b) may retard progression of early primary myelofibrosis

Silver

Vandris

2009

Leukemia

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Although heterozygous mutations in RUNX1 are not sufficient for leukemogenesis, 1,2 somatically acquired secondary events may promote transformation leading to overt MDS and AML. As seen in the reported family, recruitment of different secondary alterations may partially explain the variable penetrance and clinical heterogeneity seen in FPD/MM. Cytogenetic investigations of leukemia patients with FPD/MM displayed chromosomal aberrations that frequently occur in sporadic MDS/AML, and vice versa, RUNX1 mutations were seen in sporadic MDS/ AML. 1 Consequently, rare FPD/MM-related myeloid malignancies may serve as a model for multistep leukemogenesis in MDS/AML 8 and, as illustrated here, aCGH may help to identify candidate genes involved in malignant transformation in familial and sporadic myeloid malignancies.

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contrasting

confidence: 56%

mentioning

confidence: 99%

Recombinant interferon alpha (rIFNα-2b) may retard progression of early primary myelofibrosis

Silver

Vandris

2009

Leukemia

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“…It is now well established that IFN-a can control erythrocytosis or thrombocytosis in the majority patients with PV or ET (usual dose is 3 million units SC three times-a-week) [118]. A similar degree of benefit is appreciated in terms of reduction in spleen size or relief from pruritus.…”

Section: Annual Clinical Updates In Hematological Malignanciesmentioning

confidence: 98%

Polycythemia vera and essential thrombocythemia: 2015 update on diagnosis, risk‐stratification and management

2015

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Disease overview: Polycythemia vera (PV) and essential thrombocythemia (ET) are myeloproliferative neoplasms, respectively characterized by erythrocytosis and thrombocytosis. Other disease features include leukocytosis, splenomegaly, thrombosis, bleeding, microcirculatory symptoms, pruritus, and risk of leukemic or fibrotic transformation. Diagnosis: PV is defined by a JAK2 mutation, whose absence, combined with normal or increased serum erythropoietin level, makes the diagnosis unlikely. Differential diagnosis in ET includes reactive thrombocytosis, chronic myeloid leukemia, and prefibrotic myelofibrosis. Janus kinase 2 (JAK2), calreticulin (CALR), or myeloproliferative leukemia virus oncogene (MPL) mutations occur in approximately 55%, 25%, and 3% of ET patients, respectively. The same molecular markers are also present in prefibrotic myelofibrosis, which needs to be morphologically distinguished from ET. Survival and leukemic/fibrotic transformation: Median survivals are ∼14 years for PV and 20 years for ET; the corresponding values for younger patients are 24 and 33 years. Life‐expectancy in ET is inferior to the control population. JAK2/CALR mutational status does not affect survival in ET. Risk factors for survival in ET and PV include advanced age, leukocytosis, and thrombosis. Leukemic transformation rates at 20 years are estimated at <10% for PV and 5% for ET; fibrotic transformation rates are slightly higher. Thrombosis risk stratification: Current risk stratification in PV and ET is designed to estimate the likelihood of recurrent thrombosis: high‐risk is defined by the presence of age >60 years or presence of thrombosis history; low‐risk is defined by the absence of both of these two risk factors. Recent data consider JAK2V617F and cardiovascular risk factors as additional risk factors. Presence of extreme thrombocytosis might be associated with acquired von Willebrand syndrome (AvWS) and, therefore, risk of bleeding. Risk‐adapted therapy: The main goal of therapy in PV and ET is to prevent thrombohemorrhagic complications. In low risk patients, this is accomplished by the use of low‐dose aspirin and phlebotomy (hematocrit target <45%) in PV. In high risk (for thrombosis) patients, treatment with hydroxyurea is additionally recommended. Treatment with busulfan or interferon‐α is usually effective in hydroxyurea failures and the additional value of JAK inhibitor therapy in such cases is limited. Screening for AvWS is recommended before administrating aspirin, in the presence of extreme thrombocytosis. Am. J. Hematol. 90:163–173, 2015. © 2014 Wiley Periodicals, Inc.

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“…Since 1987, several studies have suggested that interferons (alpha or beta that are either pegylated or not) may be beneficial in the treatment of myelofibrosis (Parmeggiani et al, 1987;Kiladjian et al, 2008a). Given the efficacy of pegylated interferon a-2a (Peg-IFN a-2a) on biological and molecular parameters in polycythemia vera (PV) patients (Kiladjian et al, 2008b), we undertook a multicentre retrospective study in order to evaluate the impact of this treatment on the clinical and biological parameters inherent to myelofibrosis.…”

Section: Peg-ifn-a-2a Therapy In Patients With Myelofibrosis a Studymentioning

confidence: 99%

PEG‐IFN‐α‐2a therapy in patients with myelofibrosis

Ianotto¹,

Kiladjian

Demory

et al. 2009

Br J Haematol

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showing a complete haematological and cytogenetic conversion and a ratio of 0AE0177% at quantitative RT-PCR. As regard to B-CLL, the peripheral blood flow-cytometric analysis revealed that the percentage of clonal lymphocytes had dropped from 80% to 8% (absolute count: from 8AE33 to 0AE33 · 10 9 /l), while FISH analysis showed trisomy 12 in 7% of the 300 nuclei examined. No peripheral lymphadenopathies were detected by physical examination. Abdominal ultrasound showed the reduction of splenomegaly (13 cm diameter) and the complete disappearance of the retroperitoneal lymphadenopathies. Our clinical observation, carried out on a rare case of B-CLL associated with CML, follows the few previously reported experiences on the successful use of dasatinib in B-CLL (Pitini et al, 2009). Although in vitro dasatinib appeared to be effective mainly in cases of unmutated B-CLL (Veldurthy et al, 2008) at concentrations difficult to attain in vivo (Amrein et al, 2008), our experience suggests that it can be active also in a IGHVmutated ZAP-70 negative case, at the usual dose. Obviously, the effectiveness of dasatinib in the treatment of patients affected by B-CLL needs to be exploited in prospective studies.

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Interferon-α therapy in bcr-abl-negative myeloproliferative neoplasms

Cited by 152 publications

References 93 publications

Recombinant interferon alpha (rIFNα-2b) may retard progression of early primary myelofibrosis

Recombinant interferon alpha (rIFNα-2b) may retard progression of early primary myelofibrosis

Polycythemia vera and essential thrombocythemia: 2015 update on diagnosis, risk‐stratification and management

PEG‐IFN‐α‐2a therapy in patients with myelofibrosis

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