| Literature DB >> 12592369 |
E Passalidou1, M Stewart, M Trivella, G Steers, G Pillai, A Dogan, I Leigh, C Hatton, A Harris, K Gatter, F Pezzella.
Abstract
The few studies published on angiogenesis in lymphoma have raised the question of whether or not microvessel density (MVD) is associated with more aggressive disease and have reported the observation that in follicular lymphomas, vessels are mature rather than immature. We investigated MVD and the vascular phenotype within follicular or diffuse large B-cell lymphomas, reactive nodes and tonsils. Vascular phenotype was defined by the expression or loss of reactivity to the antibody LH39 (detecting the LH39 laminin epitope of the basement membrane in mature vessels) and by detection of alpha V beta 3 (expressed on immature vessels). In reactive nodes and in follicular lymphomas, MVD was higher in the paracortex than in germinal centres or in neoplastic follicles. However, in neoplastic follicles an increase in alpha V beta 3-positive endothelium suggested the activation of an angiogenic pathway different from that present in the reactive follicles. In large B-cell lymphomas, MVD was higher than in reactive and neoplastic follicles but lower than in the reactive paracortex. The number of immature vessels (LH39 negative) and of alpha V beta 3-positive vessels was higher than in reactive lymph nodes and follicular lymphoma suggesting that a switch to a different angiogenic pathway has occurred. Finally, we have demonstrated that within reactive and neoplastic follicles vascular regression is occurring, perhaps constraining the growth of reactive follicles alongside other phenomena such as apoptosis. Vascular regression was previously believed to occur in adults only in ovarian and endometrial tissue. We conclude that different types of angiogenesis are present in follicular lymphomas and large B-cell lymphomas. This has implications for possible future therapies.Entities:
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Year: 2003 PMID: 12592369 PMCID: PMC2377172 DOI: 10.1038/sj.bjc.6600742
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Comparison of MVD, number of mature vessels (LH39+) and putative immature vessels (αVβ3+) between follicles and paracortex in reactive hyperplasia and follicular lymphomas (paired samples t-test)
| Reactive, nodes and tonsils (17) | ||||
| MVD | 68.7 | 282.5 | <0.0009 | |
| LH39+vessels | 77.8 | 97.7 | <0.0009 | |
| | 10.2 | 22.6 | =0.044 | |
| Follicular lymphoma, All (23) | ||||
| MVD | 65.9 | 184.6 | <0.0009 | |
| LH39+vessels | 75.8 | 90.4 | <0.0009 | |
| | 45.8 | 66.1 | =0.006 | |
Comparison of MVD, number of mature vessels (LH39+) and putative immature vessels (αVβ3+) between reactive lymphoid tissue, follicular lymphomas and diffuse large B-cell lymphomas (independent samples t-test)
| MVD | 68.7 | 65.9 | =0.785 | 282.5 | 184.6 | <0.0009 | ||
| LH39+vessels | 77.8 | 75.8 | =0.689 | 97.7 | 90.4 | =0.007 | ||
| 10.2 | 45.8 | <0.0009 | 22.6 | 66.1 | <0.0009 | |||
| MVD | 185.7 | 68.7 | <0.0009 | 185.7 | 282.5 | =0.001 | ||
| LH39+vessels | 50.8 | 77.8 | =0.007 | 50.8 | 97.7 | <0.0009 | ||
| 62.7 | 10.2 | <0.0009 | 62.7 | 22.6 | <0.0009 | |||
| MVD | 185.7 | 65.9 | <0.0009 | 185.7 | 184.6 | =0.956 | ||
| LH39+vessels | 50.8 | 75.8 | =0.007 | 50.8 | 90.4 | <0.0009 | ||
| 62.7 | 45.8 | =0.019 | 62.7 | 66.1 | =0.637 |
Comparison of percentage of regressing vessels between reactive lymphoid tissue, follicular lymphomas and diffuse large B-cell lymphomas (independent samples t-test)
| Regressing vessels (%) | 10.4 | 10.1 | =0.940 | 2.1 | 0.2 | =0.223 | ||
| Regressing vessels (%) | 0.4 | 10.4 | =0.001 | 2.1 | 0.46 | =0.286 | ||
| Regressing vessels (%) | 0.4 | 10.1 | <0.0009 | 0.4 | 0.2 | =0.469 |
Figure 1Vascular phenotype in reactive and neoplastic lymph nodes. LH39-positive meshwork in (A) a reactive lymph node (B) a follicular lymphoma and (C) a large B-cell lymphoma; in the latter only a few residual fragments of the LH39 meshwork are present (arrow). (D) Reactive lymph nodes: all the vessels in the paracortex are within the LH39 meshwork while (E) LH39-negative vessels are present within a germinal centre. (F) Only rare LH39-negative vessels are seen in the paracortex in Follicular lymphomas (arrow) while (G) some more are present in the neoplastic follicles (arrows). Sequence of vascular regression: (H) A normal vessel in which the endothelial cells and the LH39-positive basal membrane are superimposed. (I) early detachment of the endothelial cells from the basal membrane. (J,K) Progressive fragmentation of both endothelial cells and basal membrane leading to vascular regression.
Comparison of percentage of regressing vessels between follicles and paracortex in reactive hyperplasia and follicular lymphomas (paired samples t-test)
| Reactive, nodes only (11) | 9.0 | 0.2 | =0.021 | |
| Reactive, nodes and tonsils (16) | 10.4 | 2.1 | =0.010 | |
| Follicular NHL all (21) | 10.1 | 0.2 | <0.0009 |
The high value reported in the paracortex of reactive tonsils is because of a single case of reactive tonsil in which 24% of the paracortical vessels showed signs of regression.
Summary of angiogenesis-related features in lymph nodes (data from the present paper, Stewart and Doussis-Anagnostopoulou )
| (A) Reactive germinal centres, neoplastic follicles and diffuse large cell NHL | |||
|---|---|---|---|
| MVD | 69.7 | 63 | |
| Mature LH39%+ | 79.6% | 76.5% | |
| LH39 meshwork | Lysis | Lysis | Lysis |
| 6.3% | |||
| Regressing vessels | 9% | 10.6% | |
| Hif1a | +21/25 (84%) | +17/30(56%) | 37/48(77%) |
| Hif2a | Mac | Mac | Mac++ |
| CA IX nuclear | Mac (several) | Mac (several) | |
| CA IX membrane | Absent | Absent | |
| VEGF | Mac | ||
| TP cells | Mac/FDR | Mac/FDR | Dendritic like cells |
| (B) Paracortex from reactive lymph nodes, paracortex in lymph nodes with follicular lymphoma and diffuse large cell NHL | |||
| MVD | 287 | ||
| Mature LH39%+ | 100% | ||
| LH39 meshwork | Present | Present | |
| 20.7% | |||
| Regressing vessels | 0.2% | 0.2% | 0.4% |
| Hif1a | Rare | Rare | 37 out of 48 cases (77%) |
| Hif2a | Several | Several | mac++ |
| CA IX nuclear | Absent | Absent | |
| CA IX membrane | Absent | Absent | |
| VEGF | Mac few | ||
| TP | Mac/IDR | Mac/IDR | Dendritic-like |