To investigate cardiac effects of imatinib at an extended follow-up (median 12.4 months), 12 chronic myeloid leukemia patients underwent cardiac screening. No significant changes on the frequency of cardiovascular signs and symptoms, electrocardiographic abnormalities, echocardiographic measurements and BNP levels were observed. Median ejection fraction was 67% at baseline versus 68% at follow-up (median intra-patient change 0.5%). Median BNP levels were 8.3 versus 7.3pg/mL (median intra-patient change 0.2pg/mL). Troponin I measures were below the lower limit of detection, whereas strain measures were similar to healthy control. This pilot study suggests that it is probably safe to perform cardiac monitoring on an annual basis.
Aim: T‐prolymphocytic leukemia (T‐PLL) is a rare disease of the elderly characterized by a high white blood cell count and organomegaly, and is currently incurable. Our aim was to elicit graft‐versus‐leukemia reactions in a patient with T‐PLL. Methods: A 52‐yr‐old woman with refractory T‐PLL underwent a nonmyeloablative regimen followed by allogeneic peripheral blood stem cell transplantation (a “minitransplant”) from her HLA‐matched sibling. Results: There was no treatment related toxicity other than neutropenia. Engraftment was successful. The patient experienced no graft‐versus‐host disease (GVHD) at any time but, on day 84 after transplantation, had a relapse in the central nervous system. Despite infusion of donor lymphocytes and intralumbar chemotherapy, she died on day 157 of systemic disease. Conclusion: The reasons why treatment may have failed are discussed (nature of disease, disease progression, treatment schedule).
10518 Background: B2001X (NCT03123939) is a multicenter global study of tisa to provide access to patients (pts) with r/r ALL including prior anti-CD19 therapy after enrollment ended in the pivotal ELIANA (NCT02435849) study. We report clinical outcomes and cellular kinetics in B2001X including pts with prior BLINA exposure or INO as bridging therapy (BT). Methods: Eligible pts ≤21 y at diagnosis with ≥2 relapse, refractory or post allogeneic transplant (alloSCT) relapse were enrolled globally. Results: As of Nov 4, 2019, 73 pts were enrolled; 67 received tisa. 91% received lymphodepletion. Among 65 pts ≥3 mo follow up (FU) or discontinued earlier (efficacy analysis set [EAS]) median FU was 9.6 mo (range [R] 0.2-16.5). Median age 10 y (R 2-33); prior alloSCT 61%; 15 pts had prior BLINA and 9 pts had INO as BT. Efficacy is summarized in Table. 13/14 relapsed pts were medullary (isolated or combined with extramedullary [EM]) and 1 EM; 9 within 6 mo including 4/5 who were CD19(+). 64% had CRS (G 3/4 13%/15%; Penn scale); 24% had neurologic events (G 3/4 9%/2%; CTCAE v4.03). 4 deaths ≤30 d: 2 early ALL progression, 1 fatal CRS with refractory ALL, 1 infection with multiorgan failure. Transgene level in peripheral blood: limited to no in vivo expansion in nonresponders (n=8) vs responders (n=42). Median duration of persistence (T last) of tisa was 272 d (R 27-379) in responders. In pts with CR/CRi, Cmax (geo-mean [CV%]) and median T last were 9260 (124) copies/µg DNA and 154 d (R 28-349), respectively, in pts who received INO as BT (n=6) vs 38,500 (215) and 273 d (R 27-379), respectively, in pts with no INO as BT (n=36). Conclusions: Outcomes in B2001X remain consistent with ELIANA. In pts with prior BLINA or INO as BT, a trend toward suboptimal outcomes was observed but should be interpreted with caution due to small n, short FU and potential confounding factors. Clinical trial information: NCT03123939. [Table: see text]
Nas duas últimas décadas, houve uma mudança radical na terapia e na evolução do mieloma múltiplo(MM), neoplasia hematológica ainda considerada fatal. As pesquisas e investimentos em medicamentos que interferem com a fisiopatogenia e com o microambiente medular estão permitindo o controle e a regressão do clone plasmocitário maligno, mudando as perspectivas da doença. A idéia nova de usar uma droga velha, a talidomida, tem-se mostrado efetiva no MM. Em 1997, apostando nos efeitos imunomoduladores e antiangiogênicos da talidomida, foram iniciados ensaios clínicos para MM refratários. A partir daí, outras ações sobre o plasmócito e microambiente medular foram eficazes contra a doença, não somente em refratários ou recaídos, mas também como terapia de indução e/ou de manutenção da remissão. No Serviço de Hematologia do Hospital de Clínicas de Porto Alegre foram acompanhados 35 portadores de mieloma múltiplo, em uso de doses baixas (100 mg) de talidomida, pelas indicações: 13-manutenção pós-TMO, 11-pós-indução, 5-recaída, 4-refratariedade e 2-terapia de indução. O estudo vigorou entre março/01 a dez/03. Os parâmetros avaliados foram: nível Hb, pico da imunoglobulina sérica ou urinária e o número de plasmócitos na medula óssea. As medidas foram tomadas pré-talidomida e após 3, 6 e 12 meses. A taxa de imunoglobulina foi o padrão ouro para avaliação de resposta. Os resultados: a dose terapêutica tolerada em 48% dos pacientes foi 100 mg; 65% dos tratados para induzir remissão (11 pacientes) apresentaram melhora entre 25%-50% no nível da imunoglobulina sérica; 87,5% daqueles que usaram para manutenção de remissão (13 pós-TMO/ 11 pós-indução) mantiveram o mesmo plateau inicial.
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