Your search keyword '"Gamallo, C."' showing total 20 results

1. Gastric Diffuse Hamartomatous Polyposis as Unique Manifestation of Peutz-Jeghers Syndrome.

Author

Ruiz-Tovar, J. and Gamallo, C.

Published

2014

2. Human papillomavirus-16 E6 variants in cervical squamous intraepithelial lesions from HIV-negative and HIV-positive women.

Author

Pérez-Gallego, L, Moreno-Bueno, G, Sarrió, D, Suárez, A, Gamallo, C, and Palacios, J

Abstract

We studied 48 human papillomavirus (HPV)-16-positive squamous intraepithelial lesions (SILs) from HIV-negative patients (16 low-grade SILs [LSILs]; 32 high-grade SILs [HSILs]) and 13 HPV-16-positive SILs from HIV-positive patients with AIDS (1 LSIL; 12 HSILs). After HPV typing, the entire HPV-16 E6 coding region was amplified and sequenced in all samples. We detected 12 HPV-16 E6 prototypes and 4 variants among the LSILs in HIV-negative patients, and 15 HPV-16 E6 prototypes and 17 HPV-16 variants in the HSIL group. The most prevalent variant of SIL types was European 350G, present in 3 and 13 cases, respectively. In 3 HSILs and no LSILs we found mixed infection by an HPV-16 E6 prototype and a variant. Two variants (1 each in LSIL and HSIL) were of non-European lineage. The only LSIL in HIV-positive patients had an HPV-16 E6 prototype; in the HSILs, we found 8 HPV-16 E6-prototypes, 4 with mixed infection with HPV-31 and 4 variants, all European 350G. The higher proportion of HPV-16 E6 variants in HSIL than in LSIL in HIV-negative patients suggests a greater risk of progression. However, further studies are needed.

Published

2001

3. Correlation of p53 oncoprotein expression with chemotherapy response in small cell lung carcinomas

Author

Rodriguez-Salas, N., Palacios, J., Moreno, G., Castro, J. de, Gonzalez-Baron, M., and Gamallo, C.

Published

2001

4. Identification of PA2.26 antigen as a novel cell-surface mucin-type glycoprotein that induces plasma membrane extensions and increased motility in keratinocytes.

Author

Scholl, F G, Gamallo, C, Vilar¿o, S, and Quintanilla, M

Abstract

PA2.26 antigen was identified as a cell-surface protein induced in epidermal carcinogenesis and skin remodeling processes. PA2.26 is expressed in carcinoma cell lines and cultured fibroblasts but absent in nontumorigenic keratinocytes. In tissues, PA2.26 is present in epithelial cells of the choroid plexus, ependyma, glomerulus and alveolus, in mesothelial cells, and in endothelia of lymphatic vessels. Biochemical characterization of PA2.26 protein and sequence analysis of the isolated cDNA demonstrate that PA2.26 antigen is a mucin-like transmembrane glycoprotein. Confocal and immunoelectron microscopy analysis in cultured cells reveal that PA2. 26 is concentrated in actin-rich microvilli and plasma membrane projections, such as filopodia, lamellipodia and ruffles, where it colocalizes with members of the ERM (ezrin, radixin, moesin) family protein. Ezrin and moesin, but not radixin, can be coimmunoprecipitated together with PA2.26 from cell lysates. Ectopic expression of PA2.26 in immortalized, nontumorigenic, keratinocytes induces an epithelial-fibroblastoid morphological conversion with increased plasma membrane extensions, concomitantly to a major reorganization of the actin cytoskeleton, redistribution of ezrin to cell-surface projections, and enhanced motility. These findings suggest an involvement of PA2.26 in cell migration.

Published

1999

5. Identification of PA2.26 antigen as a novel cell-surface mucin-type glycoprotein that induces plasma membrane extensions and increased motility in keratinocytes

Author

Scholl, F.G., Gamallo, C., Vilar?o, S., and Quintanilla, M.

Abstract

PA2.26 antigen was identified as a cell-surface protein induced in epidermal carcinogenesis and skin remodeling processes. PA2.26 is expressed in carcinoma cell lines and cultured fibroblasts but absent in nontumorigenic keratinocytes. In tissues, PA2.26 is present in epithelial cells of the choroid plexus, ependyma, glomerulus and alveolus, in mesothelial cells, and in endothelia of lymphatic vessels. Biochemical characterization of PA2.26 protein and sequence analysis of the isolated cDNA demonstrate that PA2.26 antigen is a mucin-like transmembrane glycoprotein. Confocal and immunoelectron microscopy analysis in cultured cells reveal that PA2. 26 is concentrated in actin-rich microvilli and plasma membrane projections, such as filopodia, lamellipodia and ruffles, where it colocalizes with members of the ERM (ezrin, radixin, moesin) family protein. Ezrin and moesin, but not radixin, can be coimmunoprecipitated together with PA2.26 from cell lysates. Ectopic expression of PA2.26 in immortalized, nontumorigenic, keratinocytes induces an epithelial-fibroblastoid morphological conversion with increased plasma membrane extensions, concomitantly to a major reorganization of the actin cytoskeleton, redistribution of ezrin to cell-surface projections, and enhanced motility. These findings suggest an involvement of PA2.26 in cell migration.

Published

1999

6. Relationship between ERBB2 and E-cadherin expression in human breast cancer

Author

Palacios, J., Benito, N., Pizarro, A., Limeres, M. A., Suárez, A., Gamallo, C., and Cano, A.

Abstract

A recent in vitro study has suggested that overexpression of ERBB2 may mediate breast tumour progression and metastasis by inhibiting the transcription of the E-cadherin (E-CD) gene. To test this hypothesis in human breast cancer in vivo, we studied the relationship between the expression of both molecules in 247 breast carcinomas immunohistochemically. Five ductal carcinomas in situ overexpressed ERBB2 and showed preserved E-CD expression. Forty-four of 226 infiltrating ductal carcinomas (19.47%) showed ERBB2 overexpression, and a statistically significant relationship was found between ERBB2 overexpression and high histological grade. E-CD expression was preserved in 111 cases (49.1%) and correlated with the histological grade. However, no significant relationship was found between ERBB2 and E-CD expression. None of the 16 infiltrating lobular carcinomas expressed ERBB2 or E-CD. These observations in different histological types of breast carcinoma strongly argue against a role for ERBB2 as a transcriptional regulator of E-CD expression in most human breast carcinomas in vivo.

Published

1995

7. Are genotypes of Trypanosoma cruzi involved in the challenge of chagasic cardiomyopathy?

Author

de Diego, J. A., Palau, M. T., Gamallo, C., and Penin Alegre, P.

Abstract

Abstract: Myocardial damage in Chagas' disease differs, depending on the particular Trypanosoma cruzi stock. It is reasonable to expect that the extent of phylogenetic divergence between lineages will have an impact on the biological properties of the parasite. The aim of the present work was to evaluate this impact on the cardiac damage produced by this protozoan. Heart histopathologic lesions were studied in mice infected with 15 cloned stocks of T. cruzi of various origins pertaining to 3 major clones or genotypes (19, 20, and 39) that share 3 different profiles for a given set of genetic markers. Sets of mice were infected intraperitoneally with 106 blood trypomastigotes of each of the T. cruzi clones. The macroscopy study showed a cardiac index (CI) higher than 0.6 (cardiomegaly) in 5 of the 15 stocks studied (33.33%). Inflammatory infiltrates appeared in stocks pertaining to the three genotypes studied without relation to the genetic pattern. Pseudocysts were present at higher levels (83%) in stocks pertaining to genotype 39. A lower rate could be seen in stocks pertaining to genotype 19 (50%). Only one stock pertaining to genotype 20 presented myocardial parasites (20%). Hearts were also studied for lesions in the different cardiac chambers. Inflammatory foci as well as pseudocysts appeared mainly in ventricles, with the left ventricle sharing the highest percentage of pathologic findings. In summary, in spite of the similar inflammatory pattern demonstrated for all stocks studied, the parasite's presence seemed to be related to the genotype of reference, but no relation could be demonstrated with the genetic distances.

Published

1997

8. Differential patterns of placental and epithelial cadherin expression in basal cell carcinoma and in the epidermis overlying tumours

Author

Pizarro, A, Gamallo, C, Benito, N, Palacios, J, Quintanilla, M, Cano, A, and Contreras, F

Abstract

P-cadherin (P-CD) and E-cadherin (E-CD) are expressed by keratinocytes and play an important role in skin morphogenesis. P-CD expression is restricted to the basal layer of normal epidermis, whereas E-CD is expressed in all the living layers. We have previously reported a reduced expression of E-CD in most cases of infiltrative basal cell carcinoma (BCC). In the present work we have investigated by immunohistochemistry the expression of both P-CD and E-CD in a new series of 32 patients with BCC. Most cases of superficial multicentric BCC and some nodular tumours had preserved expression of both cadherins in all tumour cells. The majority of nodular BCCs had partially reduced expression of one or both cadherins with an ordered distribution of cells showing different cadherin staining throughout the tumour mass. A severe reduction of E-CD expression with a disordered distribution of cells with different immunostaining intensity was observed in most specimens of infiltrative BCC. In contrast, P-CD expression was preserved in all cases of infiltrative BCC. These results suggest that P-CD and E-CD play different roles in the growth pattern of BCC. In addition, both anomalous P-CD expression and reduced E-CD expression were frequently observed in the spinous layer of epidermis overlying tumours. This phenomenon was significantly associated with the presence of keratinocytic atypia, which suggests that disturbed cadherin expression could be a marker of premalignant changes and/or hyperproliferative activity in human epidermis.

Published

1995

9. E-cadherin expression in basal cell carcinoma

Author

Pizarro, A, Benito, N, Navarro, P, Palacios, J, Cano, A, Quintanilla, M, Contreras, F, and Gamallo, C

Abstract

E-cadherin (E-CD) is a calcium-dependent cell-cell adhesion molecule which is expressed in almost all epithelial tissues. E-CD expression is involved in epidermal morphogenesis and is reduced during tumour progression of mouse epidermal carcinogenesis. It has been suggested that E-CD could play a role as an invasion-suppressor molecule. In the present work we have studied the E-CD expression in 31 patients with basal cell carcinoma (BCC) using an immunohistochemical technique with a monoclonal antibody (HECD-1) specific for human E-CD. E-CD expression was preserved in all specimens of superficial and nodular BCC, and was reduced in 10 of 15 infiltrative BCCs. A heterogeneous distribution of cells with different immunostaining intensity was more frequently observed in specimens of infiltrative BCC. These results suggest that E-CD might be related to the growth pattern and the local aggressive behaviour of BCC, and support the idea that E-CD might play a role as an invasion-suppressor molecule in vivo.

Published

1994

10. Ethanol intake, plasma catecholamine levels, and ST-segment changes without myocardial injury in rats with short-term ethanol consumption

Author

Fantidis, P., Del Cerro, M.J., Martinez, I., Rubio, G., Villaespesa, A.R., Gamallo, C., Leon, G., and Santodomingo, J.

Abstract

The authors studied the effect of short-term ethanol consumption on the ST-segment and the association between ST-segment changes and the amount of daily ethanol intake and levels of plasma catecholamines. The study used 63 rats (control group n = 20, study group n = 43). The rats in the study group were exposed for 6 days to progressively larger doses of ethanol followed by 15 days of continuous exposure to ethanol. At baseline an electrocardiogram (ECG) was recorded, and on day 25 the ECG was repeated and plasma catecholamine levels were measured. The animals' hearts were removed and processed for histologic study. Repolarization abnormalities were observed in 68% of the ethanol-consuming rats. Two factors differentiated the subgroup of ethanol-consuming rats with ST-segment changes from the subgroup without ST-segment changes: amount of daily ethanol intake (0.0077 +/- 0.02 mL/g/d vs 0.0058 +/- 0.019 mL/g/d) and plasma epinephrine levels (3,881 +/- 733 pg/mL vs 1,478 +/- 406 pg/mL). No myocardial damage was detected. Our results suggest that in ethanol-consuming rats, high-volume daily ethanol intake and increased plasma catecholamines may mediate changes in the ST-segment.

Published

1995

11. 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

12. Prenatal growth of the human mandibular condylar cartilage

Author

Berraquero, R., Palacios, J., Gamallo, C., de la Rosa, P., and Rodriguez, J.I.

Abstract

The question of whether the condylar cartilage possesses a growth potential like that of the long bone growth plates has been the subject of contrasting viewpoints. We have recently established that the thickness of the human tibial growth plate progressively decreases during the second half of the fetal period, but that the changes in the total human condylar thickness do not correlate with fetal age or weight. The present study examined the change in the thickness of the human mandibular condyle layers during the fetal growth of the mandible. Mandibles were obtained from autopsy of 19 human fetuses ranging in fetal age from 18 to 41 weeks. The total length of the mandible, the lengths of the mandibular body and of the ramus were measured, as well as the gonial angles. The total thickness of the condyle, and the thicknesses of the articular, progenitor, cartilage, chondroblast, and hypertrophic chondrocyte layers were measured on the central segment of central sagittal sections of the mandibular condylar cartilage. The total mandible, the corpus and the ramus lengths increased linearly with the age of the fetus and they all correlated strongly with fetal weight. However, changes in the total condylar thickness and in the thickness of the cartilage layer (chondroblast plus hypertrophic chondrocytes) did not correlate with fetal weight or mandibular length. The thickness of the articular layer increased with weight, but changes in the progenitor layer were independent of corporal and mandibular growth. These results suggest that changes in the structure of human mandibular cartilage during the prenatal period are more related to local mechanical factors and articular activity than to the general factors that are responsible for bone lengthening at the epiphyseal growth plate. (AM J ORTHOD DENTOFAC ORTHOP 1995;108:194-200.)

Published

1995

13. Fluorescence of mast cell granules in paraffin sections and cell smears induced by an N-quaternary oxazole scintillator

Author

Espada, J., Bertolesi, G., Trigoso, C., Gamallo, C., and Stockert, J.

Abstract

The N-quaternized derivative of dimethyl-POPOP (termed Q4) induces a bluish-green fluorescent reaction in mast cell granules from paraffin sections and cell smears, in addition to a previously described bluish-white fluorescent reaction in chromatin DNA. The chromatin reaction was abolished by staining the samples either with Mayer's Haematoxylin before Q4 treatment or by Q4 treatment at pH 1.5. The reaction in mast cell granules was absent after substrate methylation. The staining sequence Haematoxylin-Eosin-Q4 also worked well in paraffin sections, allowing the observation of the current histological image under bright-field illumination as well as double-colour emission under fluorescence microscopy. The sequence is proposed as a new diagnostic procedure for demonstrating mast cell granules.

Published

1995

14. A role for the E-cadherin cell-cell adhesion molecule during tumor progression of mouse epidermal carcinogenesis.

Author

Navarro, P, Gómez, M, Pizarro, A, Gamallo, C, Quintanilla, M, and Cano, A

Abstract

The expression of the cell-cell adhesion molecules E- and P-cadherin has been analyzed in seven mouse epidermal keratinocyte cell lines representative of different stages of epidermal carcinogenesis. An inverse correlation between the amount of E-cadherin protein and tumorigenicity of the cell lines has been found, together with a complete absence of E-cadherin protein and mRNA expression in three carcinoma cell lines (the epithelioid HaCa4 and the fibroblastoid CarB and CarC cells). A similar result has been detected in tumors induced in nude mice by the cell lines, where induction of E-cadherin expression takes place in moderately differentiated squamous cell carcinomas induced by HaCa4 cells, although at much lower levels than in well-differentiated tumors induced by the epithelial PDV or PDVC57 cell lines. Complete absence of E-cadherin expression has been observed in spindle cell carcinomas induced by CarB or CarC cells. P-cadherin protein was detected in all cell lines that exhibit an epithelial (MCA3D, AT5, PDV, and PDVC57) or epithelioid (HaCa4) morphology, as well as in nude mouse tumors, independent of their tumorigenic capabilities. However, complete absence of P-cadherin was observed in the fibroblast-like cells (CarB and CarC) and in spindle cell carcinomas. The introduction of an exogenous E-cadherin cDNA into HaCa4 cells, or reactivation of the endogenous E-cadherin gene, leads to a partial suppression of the tumorigenicity of this highly malignant cell line. These results suggest a role for E-cadherin in the progression to malignancy of mouse epidermal carcinogenesis. They also suggest that the loss of both E- and P-cadherin could be associated to the final stage of carcinogenesis, the development of spindle cell carcinomas.

Published

1991

15. Protective effect of Trypanosoma rangeli against infections with a highly virulent strain of Trypanosoma cruzi

Author

Zuniga, C., Palau, T., Penin, P., Gamallo, C., and Diego, J.A. de

Abstract

We investigated the protective effect of Trypanosoma rangeli against infection with Trypanosoma cruzi in animal models of various ages and with different doses of inoculum. The age of the mice and the dose of parasites determined the course of the infection. When T. cruzi was inoculated into mice after challenge with T. rangeli, parasitaemia was more controlled, mortality decreased and histopathology showed lower inflammatory infiltration and pseudocysts. This study proposes a new murine model of the protective effect of recombinant proteins of T. rangeli for possible application in the vaccines field.

Published

1997

16. Trypanosoma rangeli  : increase in virulence with inocula of different origins in the experimental infection in mice

Author

Zuñiga, C., Palau, M. T., Penin, P., Gamallo, C., and de Diego, J. A.

Abstract

Abstract: We compared two murine models of Trypanosoma rangeli infection. The same inoculum dose and age-matched hosts were used in both cases. One group was infected with trypomastigotes obtained from passages in mice and the other, with trypomastigotes obtained from cell culture after a passage in mice. We observed that trypomastigotes obtained from the in vitro cellular infection showed increased virulence in␣experimental animals, with a 70% rate of death being noted in experimental mice instead of the lack of mortality seen when in vivo-derived parasites were used. The greatest levels of parasitemia and tissual lesions in the presence of the parasite also occurred when in vitro-derived parasites were used.

Published

1997

17. Primary cranial vault lymphoma mimicking meningioma

Author

Isla, A., Alvarez, F., Gutiérrez, M., Gamallo, C., García-Blázquez, M., and Vega, A.

Abstract

Primary lymphomas of the cranial vault are rare; only six patients have been described in the literature. We report a 75-year-old woman who was admitted to our hospital after a focal seizure. CT showed a homogeneous mass which, on contrast enhancement, was similar to a meningioma. The tumour was excised and found to be a centroblastic, centrocytic non-Hodgkin's lymphoma. Treatment was completed with radiotherapy and chemotherapy.

Published

1996

18. Cancer stem cell in larynx carcinoma: Resistance or sensibility?

Author

Martín, M., Gamallo, C., Guijarro, M., Lopez, M., Leaman, O., Liñan, O., and Cerezo, L.

Published

2013

19. P.228 Thymidylate synthase expression in oral carcinoma: an immunohistochemical study about early stages.

Author

Muñoz-Guerra, M.F., Capote, A., González, R., Martos, P., Fernández-Contreras, M.E., and Gamallo, C.

Published

2006

20. Human Papillomavirus-16 E6 Variants in Cervical Squamous Intraepithelial Lesions from HIV-Negative and HIV-Positive Women.

Author

Pérez-Gallego, L, Moreno-Bueno, G, Sarrió, D, Suárez, A, Gamallo, C, and Palacios, J

Subjects

PAPILLOMAVIRUSES, EPITHELIUM, CERVIX uteri diseases, HIV-positive women, DISEASES

Abstract

Am J Clin Pathol 2001;116(1):143–148 This group studied 48 human papillomavirus (HPV)-16–positive squamous intraepithelial lesions (SILs) from HIV-negative patients [16 low-grade SILs (LGSILs) and 32 high-grade SILs (HGSILs)] and 13 HPV-16-positive SILs from HIV-positive patients with AIDS (1 LGSIL; 12 HGSILs). After HPV typing, the entire HPV-16 E6 coding region was amplified and sequenced. They detected 12 HPV-16 E6 prototypes and four variants among the LGSILs in HIV-negative patients, and 15 HPV-16 E6 prototypes and 17 HPV-16 variants in the HGSIL group. The most prevalent variant of SIL types was European 350G, present in three and 13 cases, respectively. In three HGSILs and zero LGSILs, they found mixed infection by an HPV-16 E6 prototype and a variant. Two variants (one each in LGSIL and HGSIL) were of non-European lineage. The only LGSIL in HIV-positive patients had an HPV-16 E6 prototype; in the HGSILs, they found 8 HPV-16 E6-prototypes, four with mixed infection with HPV-31 and four variants, all European 350G. The higher proportion of HPV-16 E6 variants in HGSIL than in LGSIL in HIV-negative patients suggests a greater risk of progression. Comment: I present this article because it illustrates two things: First, while HPV typing is still looking for its role in the clinical management of abnormal Pap smears and cervical intraepithelial neoplasia, it is accepted by researchers as having a great prognostic significance in cervical disease. Second, the idea of HPV variants is puzzling to a simple practitioner like me. How much like HPV-16 does something have to be for it to be considered a variant rather than a distinct subtype? On what evidence was that decided? Will there be high-risk variants and low-risk variants of high-risk types and low-risk types? When I send an HPV type now for ASCUS triage, my report comes back as “low risk, either positive or negative and high risk, either positive or negative.” If the experts are... [ABSTRACT FROM AUTHOR]

Published

2002