Your search keyword '"Piris, M. A."' showing total 12 results

1. Concordant bone marrow involvement of diffuse large B-cell lymphoma represents a distinct clinical and biological entity in the era of immunotherapy

Author

Yao, Z, Deng, L, Xu-Monette, Z Y, Manyam, G C, Jain, P, Tzankov, A, Visco, C, Bhagat, G, Wang, J, Dybkaer, K, Tam, W, Hsi, E D, van Krieken, J H, Ponzoni, M, Ferreri, A J M, Møller, M B, Winter, J N, Piris, M A, Fayad, L, Liu, Y, Song, Y, Orlowski, R Z, Kantarjian, H, Medeiros, L J, Li, Y, Cortes, J, and Young, K H

Abstract

In diffuse large B-cell lymphoma (DLBCL), the clinical and biological significance of concordant and discordant bone marrow (BM) involvement have not been well investigated. We evaluated 712 de novo DLBCL patients with front-line rituximab-containing treatment, including 263 patients with positive and 449 with negative BM status. Compared with negative BM disease, concordant BM adversely impacted overall and progression-free survival, independent of the International Prognostic Index (IPI) and cell-of-origin classification. Once BM is concordantly involved, poor prognosis was not associated with the extent of BM involvement. Conversely, patients with discordant BM showed favorable overall survival similar to stage I–II DLBCL. A BM-adjusted IPI, using three parameters: concordant BM involvement, age >60 years, and performance status >1, improves the risk stratification for DLBCL with positive BM. Intensive immunochemotherapy seemingly rendered survival benefit for patients with concordant BM, as did rituximab maintenance for the discordant BM group. Frequently revealing adverse clinical and molecular characteristics, patients with concordant BM demonstrated gene expression signatures relevant to tumor cell proliferation, migration and immune escape. In conclusion, clinical and biological heterogeneity is seen in DLBCL with positive BM but concordant BM involvement represents a distinct subset with unfavorable gene signatures, high-risk clinicopathologic features and poor prognosis.

Published

2018

2. Loss of PRDM1/BLIMP-1 function contributes to poor prognosis of activated B-cell-like diffuse large B-cell lymphoma

Author

Xia, Y, Xu-Monette, Z Y, Tzankov, A, Li, X, Manyam, G C, Murty, V, Bhagat, G, Zhang, S, Pasqualucci, L, Visco, C, Dybkaer, K, Chiu, A, Orazi, A, Zu, Y, Richards, K L, Hsi, E D, Choi, W W L, van Krieken, J H, Huh, J, Ponzoni, M, Ferreri, A J M, Møller, M B, Parsons, B M, Winter, J N, Piris, M A, Westin, J, Fowler, N, Miranda, R N, Ok, C Y, Li, Y, Li, J, Medeiros, L J, and Young, K H

Abstract

PRDM1/BLIMP-1, a master regulator of plasma-cell differentiation, is frequently inactivated in activated B-cell-like (ABC) diffuse large B-cell lymphoma (DLBCL) patients. Little is known about its genetic aberrations and relevant clinical implications. A large series of patients with de novoDLBCL was effectively evaluated for PRDM1/BLIMP-1 deletion, mutation, and protein expression. BLIMP-1 expression was frequently associated with the ABC phenotype and plasmablastic morphologic subtype of DLBCL, yet 63% of the ABC-DLBCL patients were negative for BLIMP-1 protein expression. In these patients, loss of BLIMP-1 was associated with Myc overexpression and decreased expression of p53 pathway molecules. In addition, homozygous PRDM1deletions and PRDM1mutations within exons 1 and 2, which encode for domains crucial for transcriptional repression, were found to show a poor prognostic impact in patients with ABC-DLBCL but not in those with germinal center B-cell-like DLBCL (GCB-DLBCL). Gene expression profiling revealed that loss of PRDM1/BLIMP-1 expression correlated with a decreased plasma-cell differentiation signature and upregulation of genes involved in B-cell receptor signaling and tumor-cell proliferation. In conclusion, these results provide novel clinical and biological insight into the tumor-suppressive role of PRDM1/BLIMP-1 in ABC-DLBCL patients and suggest that loss of PRDM1/BLIMP-1 function contributes to the overall poor prognosis of ABC-DLBCL patients.

Published

2017

3. Primary testicular diffuse large B-cell lymphoma displays distinct clinical and biological features for treatment failure in rituximab era: a report from the International PTL Consortium

Author

Deng, L, Xu-Monette, Z Y, Loghavi, S, Manyam, G C, Xia, Y, Visco, C, Huh, J, Zhang, L, Zhai, Q, Wang, Y, Qiu, L, Dybkær, K, Chiu, A, Perry, A M, Zhang, S, Tzankov, A, Rao, H, Abramson, J, Sohani, A R, Xu, M, Hsi, E D, Zhu, J, Ponzoni, M, Wang, S, Li, Ling, Zhang, M, Ferreri, A J M, Parsons, B M, Li, Y, Piris, M A, Medeiros, L J, and Young, K H

Abstract

Primary testicular diffuse large B-cell lymphoma (PT-DLBCL) is a unique subtype of DLBCL. The impact of rituximab on survival and patterns of treatment failure in PT-DLBCL patient remain controversial. We analyzed the clinical and biological feature of 280 PT-DLBCL cases, 64% of which were treated with rituximab-containing regimens. Although most (95%) patients achieved complete remission, a continuous risk of relapse was observed. Rituximab significantly reduced the cumulative risk of relapse (P=0.022) and improved both progression-free survival (PFS, P=0.012) and overall survival (OS, P=0.027) of PT-DLBCL patients (5-year PFS, 56% vs 36%; 5-year OS, 68% vs 48%). Central nervous system and contralateral testis were the most common sites of relapse, but other extranodal and nodal sites of relapse were also observed. Most cases of PT-DLBCL had a non-germinal center B-cell like (84%) immunophenotype and an activated B-cell like (86%) gene expression profile (GEP) subtype. The distinctive GEP signature of primary testicular lymphoma was relevant to tumor cell proliferation, dysregulated expression of adhesion molecules and immune response, likely accounting for the poor outcome. Accordingly, forkhead box P1 transcription factor (FOXP1) and T-cell leukemia/lymphoma 1 (TCL1) oncogenic activation were confirmed and predicted a significant trend of poor survival. This study provides valuable observations for better understanding of both clinical and biological features in PT-DLBCL patients.

Published

2016

4. Contribution of JAK2 mutations to T-cell lymphoblastic lymphoma development

Author

Roncero, A M, López-Nieva, P, Cobos-Fernández, M A, Villa-Morales, M, González-Sánchez, L, López-Lorenzo, J L, Llamas, P, Ayuso, C, Rodríguez-Pinilla, S M, Arriba, M C, Piris, M A, Fernández-Navarro, P, Fernández, A F, Fraga, M F, Santos, J, and Fernández-Piqueras, J

Abstract

The JAK-STAT pathway has a substantial role in lymphoid precursor cell proliferation, survival and differentiation. Nonetheless, the contribution of JAK2 to T-cell lymphoblastic lymphoma (T-LBL) development remains poorly understood. We have identified one activating TEL-JAK2 translocation and four missense mutations accumulated in 2 out of 16 T-LBL samples. Two of them are novel JAK2 mutations and the other two are reported for the first time in T-LBL. Notably, R683G and I682T might have arisen owing to RNA editing. Mutated samples showed different mutated transcripts suggesting sub-clonal heterogeneity. Functional approaches revealed that two JAK2 mutations (H574R and R683G) constitutively activate JAK-STAT signaling in γ2A cells and can drive the proliferation of BaF3-EpoR cytokine-dependent cell line. In addition, aberrant hypermethylation of SOCS3 might contribute to enhance the activation of JAK-STAT signaling. Of utmost interest is that primary T-LBL samples harboring JAK2 mutations exhibited increased expression of LMO2, suggesting a mechanistic link between JAK2 mutations and the expression of LMO2, which was confirmed for the four missense mutations in transfected γ2A cells. We therefore propose that active JAK2 contribute to T-LBL development by two different mechanisms, and that the use of pan-JAK inhibitors in combination with epigenetic drugs should be considered in future treatments.

Published

2016

5. Bounds on the PNOF5 natural geminal occupation numbers.

Author

Piris, M.

Subjects

MATHEMATICAL bounds, NONLINEAR systems, MOLECULAR orbitals, EIGENVALUES, DENSITY matrices, FERMIONS

Abstract

Abstract: The nonlinear N-representability condition obtained by Casida [2] is checked for the eigenvalues of the reconstructed two-particle reduced density matrix used in the Piris natural orbital functional 5 (PNOF5). The distinguished difference, with respect to other necessary N-representability conditions, is that the bounds on the natural geminal occupation numbers depend only on one-fermion properties, namely, the system one-particle reduced density matrix and the 1-matrix of the natural geminal associated with the eigenvalue to be bounded. It is shown that PNOF5 satisfies this N-representability necessary condition. [Copyright &y& Elsevier]

Published

2013

6. ELECTRON MICROSCOPIC STUDY OF THE LUNGS OF DECEASED PATIENTS WITH COVID-19

Author

GONZÁLEZ, A. VIDAL, MONTAÑA, A. VICENTE, PIRIS, M. CABERO, VARGAS, J.J. PAEZ, ALEN, J. FORTES, HERNÁNDEZ-MORA, M. GÓRGOLAS, ROBAGLIA, D., PINILLA, M. PIRIS, and PÉREZ, L. PRIETO

Published

2022

7. New Solids Based on B12N12Fullerenes

Author

M. Matxain, J., A. Eriksson, L., M. Mercero, J., Lopez, X., Piris, M., M. Ugalde, J., Poater, J., Matito, E., and Solà, M.

Abstract

In recent years, BN fullerenes have been synthesized experimentally. As their carbon counterparts, these BN fullerenes could be assembled in molecular solids, but this possibility has been studied little in the literature. In this work, we focus on the smallest synthesized BN fullerene, B12N12, which is built by squares and hexagons. First, the interaction between two of these fullerenes has been analyzed, using the hybrid B3LYP and MPW1PW91 density functional methods. Two different interactions have been studied in the dimer, a square facing a square (S−S) and a hexagon facing a hexagon (H−H). In both cases, a B is facing a N. The most stable dimer was found to be S−S facing, with covalent interactions between the monomers, but other dimers with weak interactions have been found as well, which opens possibilities of new systems, as in the case of fullerene dimers and solids. The solids resulting from the infinite repetition of the characterized dimers were optimized, finding two different solids, with covalent and weak interactions between monomers, respectively. The solid with covalent interactions is a nanoporous material that is more stable by around 12 eV. Because of the nanoporous character of this solid, it could be used for heterogeneous catalysis, molecular transport, and so forth. The SIESTA code with the GGA-PBE density functional method has been used for the solid-state calculations.

Published

2007

8. Conformational analysis of 3,3-disubstituted benzoylthioureas using X-ray diffraction and ab initio calculations

Author

Sosa-Albertus, M. and Piris, M.

Abstract

A study of a series of benzoylthioureas with 3,3-disubstitution has been carried out by means of theoretical calculations. X-ray diffraction data (XRD), semiempirical and ab initio Hartree–Fock calculations demonstrated that the most stable conformation for these molecules is the so-called ‘S’. Also an explanation of the high selectivity towards the S-alkylation of the systems, based on the high contribution of the sulphur atom to the HOMO in acylthioureas is given for the title compounds. Geometries were optimized at the AM1 and HF/6-31G∗levels and subsequently the results were compared with experimental XRD.

Published

2001

9. p21WAF1/CIP1AND MDM2 EXPRESSION IN NON‐HODGKIN'S LYMPHOMA AND THEIR RELATIONSHIP TO p53 STATUS: A p53+, MDM2−, p21− IMMUNOPHENOTYPE ASSOCIATED WITH MISSENSE p53 MUTATIONS

Author

VILLUENDAS, R., PEZZELLA, F., GATTER, K., ALGARA, P., SÁNCHEZ‐BEATO, M., MARTÍNEZ, P., MARTÍNEZ, J. C., MUÑOZ, K., GARCÍA, P., SÁNCHEZ, L., KOCIALKOWSKY, S., CAMPO, E., ORRADRE, J. L., and PIRIS, M. A.

Abstract

p53 is a tumour suppressor gene which is often found to be inactivated in most types of human cancer. p53 is a transcription factor, the inactivation of which may lead to significant variations in the levels of p53 downstream proteins, such as p21WAF1/CIP1and MDM2. In view of the significance of p21WAF1/CIP1and MDM2 as wild‐type (wt) p53 targets, this study was undertaken to monitor the varying expression of these proteins in non‐Hodgkin's lymphomas (NHLs) in relation to p53 gene status. A total of 57 cases of different histological types of NHL were included in this study. Proteins p53, p21and MDM2 were analysed by immunohistochemical techniques, taking the levels expressed in reactive lymphoid tissues as reference points. p53 gene point mutations (exons 5–8) were looked for using the PCR–SSCP technique and direct sequencing. Fifteen of the 57 cases studied showed 16 mutations at the p53 gene: 12 missense, one nonsense, two silent mutations, and one frameshift deletion. Most missense mutations were associated with high levels of p53 protein, while the nonsense mutations and frameshift deletion did not induce detectable levels of p53. All cases with mutation at the p53 gene (15) showed null or low levels of p21WAF1/CIP1and MDM2 proteins, suggesting that null or missense mutations at this gene give rise to a protein that is unable to transactivate the p21WAF1/CIP1and MDM2 genes. The association between missense p53 mutation and dissociate immunophenotype (p53+, MDM2−, p21−) was statistically significant (Fisher's exact test, P=0·0024). This anomalous p53+, MDM2−, p21− phenotype was also found in a small group of five cases with wt p53; this could indicate that in these cases p53 transactivation capacity has been abrogated by a mechanism other than p53 mutation. Most cases with the wt p53 gene show simultaneous immunohistochemical expression of all three proteins and often display higher levels than those found in reactive lymphoid tissue. There is a tendency for EBV‐positive cases to harbour high levels of p53+ and p21+, suggesting that EBV could be involved in the nuclear accumulation of p53 and p21WAF1/CIP1in NHL. © 1997 by John Wiley & Sons, Ltd.

Published

1997

10. Lennert's Lymphoma with Giant Multivesicular Lysosomal Bodies Optically Visible

Author

Oliva, H., Rivas, C., Vicente, J., Aguilera, B., Rivas, F., Obeso, G., Piris, M. A., and Battifora, H.

Abstract

A case of a 43-year-old male patient with lym-phoepithelioid lymphoma is discussed. During the 10-year follow-up of this patient, different biopsy specimens were obtained. Immunohistochemical studies with a complete paraffin panel determined a T-cell nature of the specimens. Electron microscopy showed a peculiar finding in the cytoplasms of the tumoral cells that correlated with optical inclusions observed in optical imprints; these imprints corresponded to lysosomic multivesicular bodies, whose significance is discussed.

Published

1992

11. p21<SUP>WAF1/CIP1</SUP> AND MDM2 EXPRESSION IN NON-HODGKIN'S LYMPHOMA AND THEIR RELATIONSHIP TO p53 STATUS: A p53+, MDM2−, p21− IMMUNOPHENOTYPE ASSOCIATED WITH MISSENSE p53 MUTATIONS

Author

VILLUENDAS, R., PEZZELLA, F., GATTER, K., ALGARA, P., SÁNCHEZ-BEATO, M., MARTÍNEZ, P., MARTÍNEZ, J. C., MUÑOZ, K., GARCÍA, P., SÁNCHEZ, L., KOCIALKOWSKY, S., CAMPO, E., ORRADRE, J. L., and PIRIS, M. A.

Abstract

p53 is a tumour suppressor gene which is often found to be inactivated in most types of human cancer. p53 is a transcription factor, the inactivation of which may lead to significant variations in the levels of p53 downstream proteins, such as p21^WAF1/CIP1 and MDM2. In view of the significance of p21^WAF1/CIP1 and MDM2 as wild-type (wt) p53 targets, this study was undertaken to monitor the varying expression of these proteins in non-Hodgkin's lymphomas (NHLs) in relation to p53 gene status. A total of 57 cases of different histological types of NHL were included in this study. Proteins p53, p21and MDM2 were analysed by immunohistochemical techniques, taking the levels expressed in reactive lymphoid tissues as reference points. p53 gene point mutations (exons 5–8) were looked for using the PCR–SSCP technique and direct sequencing. Fifteen of the 57 cases studied showed 16 mutations at the p53 gene: 12 missense, one nonsense, two silent mutations, and one frameshift deletion. Most missense mutations were associated with high levels of p53 protein, while the nonsense mutations and frameshift deletion did not induce detectable levels of p53. All cases with mutation at the p53 gene (15) showed null or low levels of p21^WAF1/CIP1 and MDM2 proteins, suggesting that null or missense mutations at this gene give rise to a protein that is unable to transactivate the p21^WAF1/CIP1 and MDM2 genes. The association between missense p53 mutation and dissociate immunophenotype (p53+, MDM2−, p21−) was statistically significant (Fisher's exact test, P=0·0024). This anomalous p53+, MDM2−, p21− phenotype was also found in a small group of five cases with wt p53; this could indicate that in these cases p53 transactivation capacity has been abrogated by a mechanism other than p53 mutation. Most cases with the wt p53 gene show simultaneous immunohistochemical expression of all three proteins and often display higher levels than those found in reactive lymphoid tissue. There is a tendency for EBV-positive cases to harbour high levels of p53+ and p21+, suggesting that EBV could be involved in the nuclear accumulation of p53 and p21^WAF1/CIP1 in NHL. © 1997 by John Wiley & Sons, Ltd.

Published

1997

12. Ultrastructure of 26 Cases of Ki-1 Lymphomas: Morphoimmunologic Correlation

Author

Rivas, C., Piris, M. A., Gamallo, C., Barat, A., Echezarreta, G., Oliva, H., Sarasa, J. L., Rivas, F., Renedo, G., Martin, C., and Stein, H.

Abstract

Twenty-six cases of high-grade lymphomas with activation markers (CD30) classified and immunophenotyped according to the Kiel classification were studied to determine their fine structural features. Transmission electron microscopy showed in 17 cases anaplastic nuclear and cytoplasmic changes identical to those observed in Hodgkin's disease, it being impossible to determine by the morphology a B, T, or null nature. Four high-grade B-centroblastic and immunoblastic cases and five T-pleomorphic cases showed nuclear changes and cytoplasmic differentiation that suggested a T or B nature. An immunogold-labeling technique showed CD30-positive particles primarily in the Golgi complex and occasionally in the cell membrane.

Published

1990