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16. Characterization of two novel cell lines, DERL-2 (CD56+/CD3+/Tcry5+) and DERL-7 (CD56+/CD3-/TCRgammadelta-),derived from a single patient with CD56+ non- Hodgkin's lymphoma

17. characterisation of two novel cell lines, DERL-2 (CD56+/CD3+/TCR gammadelta+) and DERL-7 (CD56+/CD3-/TCR gammadelta-) derived from a single patient with CD56+ non Hodgkin lymphoma

18. Immunophenotypic analysis enables the correct prediction of t(8;21) in acute myeloid leukaemia

24. Evaluation of the platelet counting by Abbott CELL-DYN® SAPPHIRE™ haematology analyser compared with flow cytometry.

25. Characterization of two novel cell lines, DERL-2 (CD56+/CD3+/Tcry5+) and DERL-7 (CD56+/CD3-/TCRgammadelta-), derived from a single patient with CD56+ non-Hodgkin's lymphoma.

26. In vitro exposure of acute promyelocytic leukemia cells to arsenic trioxide (As[sub 2]O[sub 3]) induces the solitary expression of CD66c (NCA-50/90), a member of the CEA family.

27. JURL-MK1 (c-kit(high)/CD30-/CD40-) and JURL-MK2 (c-kit(low)/CD30+/CD40+) cell lines: 'two-sided' model for investigating leukemic megakaryocytopoiesis.

29. Multicomponent Donation of Red Blood Cells, Platelets and Plasma.

30. Complete remission in acute myeloid leukaemia with t(8;21) following treatment with G-CSF: flow cytometric analysis of in vivo and in vitro effects on cell maturation

31. CMRL-T, a novel T-cell line showing asynchronous phenotype (CD34(+)/CD1a(-)/TCRalphabeta(+)) and dual T-cell receptor beta chain

32. In vitro exposure of acute promyelocytic leukemia cells to arsenic trioxide (As2O3) induces the solitary expression of CD66c (NCA-50/90), a member of the CEA family

33. CD66c antigen expression is myeloid restricted in normal bone marrow but is a common feature of CD10+ early-B-cell malignancies

34. Differential regulation of GPI-linked molecules on leukaemic promyelocytes treated in vitro with all-trans retinoic acid

35. Stem cell factor receptor (c-kit, CD117) is expressed on blast cells from most immature types of acute myeloid mallignancies but is also a characteristic of a subset of acute promyelocytic leukaemia

36. All-trans retinoic acid (ATRA) and the regulation of adhesion molecules in acute myeloid leukemia

37. Expression of the leucocyte common antigen (LCA, CD45) isoforms RA and RO in acute haematological malignancies: possible relevance in the definition of new overlap points between normal and leukaemic haemopoiesis

38. All-trans retinoic acid promotes a differential regulation of adhesion molecules on acute myeloid leukaemia blast cells

39. Expression and ATRA-driven modulation of adhesion molecules in acute promyelocytic leukemia

40. Co-ordinate expression of T-cell antigens on acute myelogenous leukemia and of myeloid antigens on T-acute lymphoblastic leukemia. Speculation on a highly balanced bilinearity

41. Immunodiagnosis of acute leukemia displaying ectopic antigens: Proposal for a classification of promiscuous phenotypes

42. Surface mu chains in acute lymphoblastic leukemia: a new 'early B' phenotype

43. Features, reason for testing, and changes with time of 583 paroxysmal nocturnal hemoglobinuria clones from 529 patients: a multicenter Italian study.

44. Extended flow cytometry characterization of normal bone marrow progenitor cells by simultaneous detection of aldehyde dehydrogenase and early hematopoietic antigens: implication for erythroid differentiation studies.

45. CMRL-T, a novel T-cell line showing asynchronous phenotype (CD34(+)/CD1a(-)/TCRalphabeta(+)) and dual T-cell receptor beta chain.

46. Presence of FLT3 mutations does not impair stem cell mobilization and feasibility of autologous peripheral blood stem cell transplantation in acute myeloid leukemia.

47. Complete remission in acute myeloid leukaemia with t(8;21) following treatment with G-CSF: flow cytometric analysis of in vivo and in vitro effects on cell maturation.

49. All-trans retinoic acid (ATRA) and the regulation of adhesion molecules in acute myeloid leukemia.

50. Expression of the leucocyte common antigen (LCA, CD45) isoforms RA and RO in acute haematological malignancies: possible relevance in the definition of new overlap points between normal and leukaemic haemopoiesis.

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