ALBERT

Description: Abstract 4620 Myelodysplastic syndrome (MDS) is a clonal hematopoietic stem cell disorder characterized by dyshematopoiesis and high susceptibility to acute myeloid leukemia. Deregulated epigenetic mechanisms are likely involved in the pathogenesis of MDS. Gene silencing through aberrant CpG island methylation is the most extensively analyzed epigenetic event in human tumorigenesis and has huge diagnostic and prognostic potential. Aberrant methylation of gene promoter region is responsible for inappropriate gene silencing, and it has been associated to initiation and progression of cancer. However, in the MDS disease process, more and more gene dysfunction has been related with the pathogenesis. FLT3 and c-KIT are important members of the receptor tyrosine kinase family that are overexpress or dysexpress in many malignant hematologic diseases. However, little is known about the distribution and the role of these proteins in MDS. The study is to investigate the role of receptor tyrosine kinase FLT3 and c-KIT expression in patients with myelodysplastic syndromes (MDS) and their clinical implication. We have at moment examined c-kit protein (CD117) expression by flow cytometry, in CD34 bone marrow cells collected at diagnosis of 12 patients with de novo MDS and 5 non-neoplastic patients (controls). FLT3 mutations, in particular Internal Tandem Duplications (ITD) and the D835 mutation were analysed by PCR-RFLP. The median age was 72 years (22–89), gender M/F=5/7, WHO subtypes: RCMD (n=6), RA (n=3), RARS (n=1), AREB-2 (n=1), CMML (n=1) and IPSS: low (n=6), intermediate-1 (n=5) and intermediate-2 (n=1). None of the patients evolved to acute leukemia, with a median follow up of 24 months (7–74). Our preliminary results show an increase in c-KIT expression in CD34 positive cells in MDS patients as compared with controls. However, the percentage of c-KIT protein expressing cells was also higher than in the controls in particular in CD34 negative cells. There was a correlation of the c-kIT protein expression with the CD34 antigen of the cells. Expression is correlated with the WHO MDS classification and with IPSS, being highest in RAEB-2 and INT2 MDS prognostic group. These results suggest that the elevated c-KIT expression could maintain the affected clone in MDS. Besides that we didn't find any FLT3 mutations in our population However further data and refinement of data analysis are needed to confirm our results and to predict clinical outcomes. The preliminary results suggest that c-KIT expression could be helpful to the pathogenesis and prognosis prediction of MDS patients. Disclosures: No relevant conflicts of interest to declare.

Description: Abstract 5094 Background: Triclonal patterns (TP) in immunofixation (IF), characterized by the presence of three different immunoglobulin bands, are a very rare finding: we have recently reported an incidence of 0.1% (representing 0.82% of all clonal patterns detected), in 0.1% of patients tested, in an 11-year series of 46 249 immunofixation essays, collected from 29 704 patients. We found that for the majority of patients (56.2%) triclonality in IF was a transient feature, with patients acquiring TP and de-escalating to biclonality or monoclonality, and suggested that transiency could be a feature of clonal evolution, involution and selection. Such clonal modifications could be induced by chemotherapy (CHTx) or bone marrow transplant or, on the other hand, could also be an indication of disease progression. The presence of TP could also be an intrinsic spontaneous characteristic of the patient or the disease. Aims: This study aims to clarify whether TP should be interpreted as merely an artifact of ongoing therapy, or if it could be deserving of attention by the clinician, by studying the relationship between the identification of TP in IF in multiple myeloma (MM) and monoclonal gammopathy of undetermined significance (MGUS) patients and the timing of treatment. Methods: We identified all samples exhibiting a TP among the 47 559 IF essays performed in our center from January 2000 to June 30th 2011. We found 53 sera with TP, from 35 patients, two of whom were external consultation referrals and, therefore, excluded from our analysis. We also excluded an HIV-positive patient who died within 5 days of a single triclonal IF, a liver transplant recipient undergoing immunosuppression, 2 patients with isolated TP during respiratory infections, 3 lymphomas (one marginal zone lymphoma and 2 follicular lymphomas) presenting with TP during CHTx and a renal transplant recipient who acquired a TP and 4 months later was diagnosed with NHL, dying within 10 days. Results: Of the 25 remaining patients with MM and MGUS, we recognized a spontaneous development of triclonality at diagnosis, prior to the institution of any treatment, in 28% (7 patients). One patient with MM had a single triclonal IF, and died within 30 days of the presenting symptoms; one maintained the same TP pattern throughout therapy; one MM and one MGUS, both recent diagnoses, have yet to have follow-up IF; the remaining 3 MM patients lost their TP spontaneously (1 patient) or during treatment (2 patients). An additional 8% (2 patients with MM) had a diagnosis established outside of our centre, with no description of triclonality; the first IF performed in our Hospital had a TP, before the start of therapy, and both lost their TP with treatment. Five patients (20%) acquired a TP spontaneously after diagnosis, but prior to any therapy. Two MGUS later spontaneously lost their TP; one MM lost it with therapy; one patient had MGUS for 3 years before acquiring an inconstant TP, which he subsequently lost after 6 years, progressing to MM one year later; one patient with an indolent myeloma, developed a TP 6 years after diagnosis, on progression to symptomatic myeloma. The remaining 44% (11 patients) acquired their TP only after the introduction of therapy. This includes 5 MM after CHTx (4 after thalidomide-containing regimens), 4 MM after autologous hematopoietic stem cell transplantation, one Waldenström's macroglobulinemia and one patient with essential thrombocytosis and MGUS who acquired TP after starting hydroxicarbamide. Discussion: In this series we found that 28 to 36% of patients with a TP presented with this pattern upon diagnosis, prior to any therapy, with a further 20 to 28%, who were not triclonal at the outset, acquiring it spontaneously without treatment. Therefore, for 56% of patients, triclonality – though frequently transient – is a feature of their disease. On the other hand, for the remaining 44% of patients, the appearance of a TP is temporally associated with CHTx or transplantation (though it is impossible to affirm that the patients would not have acquired the patterns in the absence of CHTx). Conclusions: We conclude that the appearance of a TP on IF, through rare and in most cases transient, should not be discarded as a mere effect of treatment. In over half the cases, there is no association between triclonality and treatment; the clinician should, therefore, interpret the results on a case-by-case basis, as the acquisition of TP could be a marker of disease progression. Disclosures: No relevant conflicts of interest to declare.

Description: Malaria is one of the most frequent hemoparasitic infections in developing countries, responsible for a high health burden; with increasing world travel, growing numbers of patients present with malaria in non-endemic areas. While the clinical presentation of malaria is well characterized in the literature, it is non-specific, and suspicion is often raised simply by a fever and a report of a recent stay in an endemic area. Due to the connection of Europe with its former colonies, with bilateral migratory patterns, this anamnestic suspicion is frequent. To determine whether the addition of classic malaria hematology findings (thrombocytopenia, anemia and increased serum lactate dehydrogenase – LDH - levels) can improve clinical suspicion in patients presenting in non-endemic countries, We reviewed all malaria testing resulting from emergency room (ER) visits between 01-01-2000 and 06-30-2013. Repeated tests related to the same ER visit were analysed together; patients with more than one unrelated ER visit with suspected malaria were treated as separate subjects. Results 1357 subjects (69.0% male) fulfilled our criteria (median of 96 per year); the percentage of yearly Positive results varied between 2.6 and 17.0%, with no discernible temporal pattern, for an overall average of 9.5% of Positives. The monthly distribution of testing was balanced, with each month accounting for 6.4 to 10.2% of yearly tests; however, the percentage of Positives had a bimodal distribution, with two significant peaks in April (14.3% positivity) and December (16.5%); males were twice as likely to be Positive (11.0 vs 6.2%, p=0.005). There was a significant decrease in the mean haemoglobin of malaria-Positive patients (12.8±2.6 vs 13.5±2.2 g/dL, p