IntroductionMultiple myeloma (MM) remains an incurable disease, despite conventional and high-dose chemotherapies. 1 Molecules targeting not only plasma cells, but also the bone marrow (BM) microenvironment are needed to overcome drug resistance.Pathologic angiogenesis is a constant component of the MM microenvironment. 2 The vascular endothelial growth factor (VEGF)/ VEGF receptor-2 (VEGFR-2) pathway greatly contributes to MM angiogenesis and growth, 3 and mediates proliferation and capillarogenesis in MM endothelial cells (MMECs) through an autocrine loop. 4 VEGF 165 is the most abundant and effective isoform. 5 It binds simultaneously to its cognate receptors VEGFR-1 and VEGFR-2 and to the coreceptor neuropilin-1 (NRP1), a cellsurface glycoprotein expressed on axons in the developing nervous system as well. 6 NRP1 is the ligand-binding subunit of the receptor complex for class 3 semaphorins, a family of secreted proteins that mediate neuronal guidance. 7 Binding of secreted semaphorin 3A (SEMA3A) to NRP1 induces the collapse of neuronal growth cones 8 by activating the signal-transducing subunit(s) of the receptor complex, that is, class A plexins, a family of transmembrane proteins whose cytoplasmic domain is endowed with an R-Ras GAP activity that inhibits integrin function. 9 NRP1 is also expressed on ECs, 10 where it acts as an isoform-specific receptor for VEGF 165 , and enhances by 4-to 6-fold its affinity for VEGFR-2, as well as VEGF 165 -induced cell chemotaxis and proliferation. 11 By competing with VEGF 165 for binding to NRP1 12 and by activating class A plexins, 13 SEMA3A inhibits integrinbased EC adhesion and migration and capillary sprouting. Autocrine loops of endothelial SEMA3A play a self-limiting role in angiogenesis and regulate EC behavior during its physiologic development. 13 Here we analyze the expression levels of VEGF 165 , SEMA3A, and their receptors NRP1 and plexin-A1 in BM ECs isolated from patients with MM and MGUS (MMECs and MGECs), and from the human umbilical vein (HUVECs). We show that overangiogenic MMECs display a high VEGF 165 /SEMA3A ratio and behave like MGECs and HUVECs upon exposure to exogenous SEMA3A, which seems as effective as an anti-VEGFR-2 antibody. Our observations point to SEMA3A as a potential antiangiogenic
Patients, materials, and methods
PatientsThirty-two patients fulfilling the International Myeloma Working Group diagnostic criteria 14 for MM (n ϭ 18) and MGUS (n ϭ 14) were studied at diagnosis. The MM patients (12 male, 6 female) were aged 44 to 81 years (median 68.5 years) and staged 15 as IIA (n ϭ 4), IIB (n ϭ 2), IIIA (n ϭ 10), and IIIB (n ϭ 2); the M-component was IgG (n ϭ 12), IgA (n ϭ 4), and or (n ϭ 2). The MGUS patients (8 male, 6 female) were aged 42 to 79 years (median 70.6 years) and were IgG (n ϭ 10) or IgA (n ϭ 4). The study was approved by the local ethics committee of the University of Bari Medical School, Italy, and all patients gave their informed consent in accordance with the Declaration of Helsinki.
Separation and culture of ECs and...