Your search keyword '"Scapoli, Luca"' showing total 29 results

1. Cleft lip with or without cleft palate: implication of the heavy chain of non-muscle myosin IIA

Author

Martinelli, Marcella, Di Stazio, Mariateresa, Scapoli, Luca, Marchesini, Jlenia, Di Bari, Filomena, Pezzetti, Furio, Carinci, Francesco, Palmieri, Annalisa, Carinci, Paolo, and Savoia, Anna

Subjects

Cleft lip -- Genetic aspects, Cleft lip -- Development and progression, Cleft lip -- Research, Myosin -- Genetic aspects, Myosin -- Analysis, Health

Published

2007

2. Allogro[R] acts on stem cells derived from peripheral blood

Author

Sollazzo, Vincenzo, Palmieri, Annalisa, Scapoli, Luca, Martinelli, Marcella, Girardi, Ambra, Pellati, Agnese, Scarano, Antonio, Perrotti, Vittoria, Spinelli, Giuseppe, and Carinci, Francesco

Subjects

Stem cells -- Physiological aspects, Stem cells -- Research, Artificial bones -- Usage, Artificial bones -- Health aspects, Bone-grafting -- Health aspects, Oral surgery -- Health aspects, Health, Allogro (Orthopedic apparatus) -- Usage, Allogro (Orthopedic apparatus) -- Health aspects

Abstract

Introduction: Allogro [R] is a demineralized freeze-dried bone allograft, a promising material for bone grafting, which is useful as a scaffold to fill bone defects and to restore bone loss in orthopedic and maxillofacial surgery.However, how Allogro [R] alters osteoblast activity to promote bone formation is poorly understood.Materials and Methods: To study how Allogro [R] can induce osteoblast differentiation in mesenchymal stem cells, the expression levels of bone related genes and mesenchymal stem cells marker were analyzed, using real time Reverse Transcription-Polymerase Chain Reaction.Results: Allogro [R] causes a significant induction of osteoblast transcriptional factor like osterix (RUNX2) and of the bone related genes osteopontin (SPP1), osteocalcin (BGLAP) and alkaline phosphatase (ALPL).Conclusion: The obtained results can be relevant to better understand the molecular mechanism of bone regeneration and as a model for comparing other materials with similar clinical effects. Keywords: stem cell | biomaterial | Allogro [R] | differentiation | bone, Introduction The increase in orthopedic and dental prosthetic surgery is often associated with the need to restore the bone loss subsequent prosthetic failure and osteolysis resulting from wear particles of [...]

Published

2009

3. Association between TGFB3and Nonsyndromic Cleft Lip with or Without Cleft Palate in a Chilean Population

Author

Suazo, José, Santos, José Luis, Scapoli, Luca, Jara, Lilian, and Blanco, Rafael

Abstract

Objective To assess the possible association between TGFB3allele variants and nonsyndromic cleft lip with or without cleft palate in a Chilean population.Design In our study we used a case-parents trios design. The sample consisted of 150 unrelated trios ascertained through probands affected with nonsyndromic cleft lip with or without cleft palate. Three TGFB3polymorphisms were analyzed (rs2268626, rs2268625, and rs3917201). An allele/haplotype transmission disequilibrium test was used to evaluate the possible genotype-phenotype association.Results An overtransmission from parents to affected progeny was observed for the A allele of rs3917201 (p= .03) and for the rs2268625-rs3917201 A-A haplotype (p= .022). A defect of transmission of rs2268625-rs3917201 G-G haplotype (p= .022) was observed also.Conclusions Allelic and haplotypic associations implicate a possible role of TGFB3in nonsyndromic cleft lip with or without cleft palate in the Chilean population. Additional studies are needed in order to elucidate the possible mechanisms that can explain the role of TGFB3genetic variants in the condition.

Published

2010

4. New Insights in Collagen Turnover in Orofacial Cleft Patients

Author

Gagliano, Nicoletta, Carinci, Francesco, Moscheni, Claudia, Torri, Carlo, Pezzetti, Furio, Scapoli, Luca, Martinelli, Marcella, Gioia, Magda, and Stabellini, Giordano

Abstract

Objective We aimed to characterize the fibroblast phenotype of patients by analyzing gene and protein expression of cleft lip and/or cleft palate fibroblasts in relation to collagen turnover and extracellular matrix remodeling.Patients Human palatal fibroblasts were obtained from three healthy subjects without cleft lip and/or cleft palate and from three subjects with nonsyndromic cleft lip and/or cleft palate. Collagen turnover–related gene and protein expression were analyzed by real-time polymerase chain reaction, Western and dot blots, and sodium dodecyl sulfate zymography.Results Cleft lip and/or cleft palate fibroblasts, compared with controls, displayed a down-regulation of collagens type I and III messenger RNA (p< .0001 and p< .001, respectively) but an opposite tendency to increase protein levels. Cleft lip and/or cleft palate cells had higher lysyl hydroxylase-2b messenger RNA levels expressed in relation to collagen type I messenger RNA, down-regulated matrix metalloproteinase-1, tissue inhibitor of matrix metalloproteinase-1, and Secreted Protein Acidic and Rich in Cysteine messenger RNA (p< .0001 and p< .01, respectively). Pro–matrix metalloproteinase-1 tended to decrease, and pro–matrix metalloproteinase-2 and -9 were down-regulated (p< .01, p< .05, respectively), as was Secreted Protein Acidic and Rich in Cysteine protein expression (p< .05).Conclusions Our results suggest that the cleft lip and/or cleft palate fibroblast phenotype is characterized by a tendency toward interstitial collagen deposition due to posttranslational modifications, such as decreased collagen degradation by matrix metalloproteinases and increased collagen cross-links. These findings may contribute to the knowledge of the cleft lip and/or cleft palate fibroblast phenotype and may be useful to the surgeon when considering the potential wound contraction and subsequent undesired scarring in cleft lip and/or cleft palate ocurring after the surgical closure of a cleft palate.

Published

2010

5. Low prevalence of human papillomavirus in squamous-cell carcinoma limited to oral cavity proper

Author

Scapoli, Luca, Palmieri, Annalisa, Rubini, Corrado, Martinelli, Marcella, Spinelli, Giuseppe, Ionna, Franco, and Carinci, Francesco

Abstract

Several investigations have reported that the human papillomavirus may play a role in head and neck squamous-cell carcinoma development and may have a prognostic impact. However, inconsistent results regarding human papillomavirus prevalence have been obtained so far. Variables which may account for these discrepancies may be related to site of the samples' origin, detection methods and sample size. The aim of this study is to evaluate the presence of high-risk type human papillomavirus in a large, well defined sample of squamous-cell carcinoma limited to the oral cavity in its strictest definition—ie with no pharynx or larynx cancers included—by means of quantitative real-time polymerase chain reaction, a method which ensures high sensitivity and offers the opportunity to exclude false-positive results. Data were obtained from 314 squamous-cell carcinoma limited to oral cavity proper, indicated that the prevalence of high-risk human papillomavirus was as low as 2% (CI 0.6–3). Matched pairs case-control analysis indicated that the prevalence among controls did not significantly differ with respect to cases and thus did not support a major role for the human papillomavirus in the etiology of squamous-cell carcinoma of the oral cavity.

Published

2009

6. Comparison Between Genetic Portraits of Osteoblasts Derived From Primary Cultures and Osteoblasts Obtained From Human Pulpar Stem Cells

Author

Carinci, Francesco, Papaccio, Gianpaolo, Laino, Gregorio, Palmieri, Annalisa, Brunelli, Giorgio, D'Aquino, Riccardo, Graziano, Antonio, Lanza, Vladimiro, Scapoli, Luca, Martinelli, Marcella, and Pezzetti, Furio

Abstract

Harvesting bone for autologous grafting is a daily problem encountered by craniofacial and oral surgeons. Stem cells derived from human dental pulp are able to differentiate in osteoblasts and are a potential source of autologous bone produced in vitro. However, as stem cells are characterized by self-renewing and commitment in several cellular subtypes (ie, pluripotential differentiation), some concerns may arise as regards their potential uncontrolled proliferation.

Published

2008

7. TGF Alpha Has Low Protein Expression in Nonsyndromic Clefts

Author

Rullo, Rosario, Gombos, Fernando, Ferraraccio, Franca, Farina, Antonio, Morano, Danila, Festa, Vincenzo, Del Viscovo, Daniele, Palmieri, Annalisa, Martinelli, Marcella, Scapoli, Luca, Pezzetti, Furio, and Carinci, Francesco

Abstract

Genetic studies have demonstrated that nonsyndromic cleft is composed of two separate entities the cleft palate only and cleft of the lip, alveolus with or without cleft palate; both have a heterogeneous genetic background and environmental factors contribute to the onset of these malformations. The role of transforming growth factor alpha (TGF-A) was considered possible, but conflicting results have been reported. To detect if TGF-A is involved in the onset of cleft diseases, a series of patients with nonsyndromic clefts and control subjects were analyzed with regard to protein expression. Forty-three patients with nonsyndromic clefts and 21 unaffected subjects were enrolled in this study. Paraffin-embedded specimens were matched with TGF-A antibody and then scanned with a computerized image analyzer. TGF-A was scored as absent, moderately (from 10% to 30%), and highly expressed in epithelium, gland, and muscle. Data were statistically analyzed with a Kruskal-Wallis test. Comparison between control subjects and patients with clefts showed that only gland and epithelium reached a significant Pvalue. A subsequent comparison between cleft of the lip, alveolus with or without cleft palate and cleft palate only groups demonstrated a statistically significant difference only for gland. TGF-A was decreasingly expressed in unaffected, cleft of the lip, alveolus with or without cleft palate, and patient with cleft palate only and thus further strength has been given to its role in the onset of the disease.

Published

2007

8. Genetic Profiling of Central Giant Cell Granuloma of the Jaws

Author

Carinci, Francesco, Piattelli, Adriano, Martinelli, Marcella, Palmieri, Annalisa, Rubini, Corrado, Fioroni, Massimiliano, Scapoli, Luca, Laino, Gregorio, Caputi, Sergio, Becchetti, Alessio, and Pezzetti, Furio

Abstract

Central giant cell granuloma (CGCG) of the jaws is a central osteolytic lesion characterized histologically by multinucleated giant cells in a background of ovoid to spindle-shaped mesenchymal cells. Whether CGCG is a reactive lesion or a truly benign neoplasm remains undetermined, and the mechanism determining the onset of the disease remains unknown. To have more information regarding the genetic events involved in CGCG, the authors decided to perform an expression profile. Samples were derived from two surgically resected CGCG of the mandible. RNA extracted from a pool of three normal bone tissues was used as control. By using DNA microarrays containing 19,200 genes, the authors identified several genes whose expression was significantly up- or down-regulated. The differentially expressed genes cover a broad range of functional activities: cell cycle regulation; signal transduction; and vesicular transport. It was also possible to detect some genes whose function is unknown. The authors believe the data reported to be the first genetic portrait of CGCG of the jaws. Several markers have been identified that can potentially help in identifying some biological behavior (ie, quiescent versus aggressive lesions), as well as genes whose products could be potentially disease-specific targets for therapy. However, the authors think that more cases are needed, especially those comparing quiescent and aggressive lesions, before the exact profile of CGCG is known.

Published

2005

9. Genetic Profiling of Granular Cell Myoblastoma

Author

Carinci, Francesco, Piattelli, Adriano, Rubini, Corrado, Fioroni, Massimiliano, Stabellini, Giordano, Palmieri, Annalisa, Scapoli, Luca, Laino, Gregorio, Muzio, Lorenzo Lo, Caputi, Sergio, Becchetti, Alessio, and Pezzetti, Furio

Abstract

Granular cell tumor (GCT), or granular cell myoblastoma, is a relatively uncommon lesion of the soft tissues. It can occur in any organ, and the tongue is more often affected. GCT has unknown etiology, uncertain histogenesis, and a not always benign nature. Benign myoblastomas are the great majority, but rare malignant lesions have been reported. To have more information regarding the genetic events involved in GCT, the authors decided to perform an expression profile. A sample was derived from a surgically resected GCT of the tongue. RNA extracted from normal tongue (mucosa plus muscle) was used as control. By using DNA microarrays containing 19,200 genes, the authors identified several genes for which expression was significantly up- or down-regulated. The differentially expressed genes cover a broad range of functional activities (1) signal transduction, (2) cell cycle regulation, and (3) cytoskeleton organization. It was also possible to detect some genes whose function is unknown. The data reported are, to the authors’ knowledge, the first genetic portrait of GCT. Mutations in some of the described genes are related to neural alterations and mental diseases, and this fact supports the idea of a neural origin of myoblastoma. Several markers have been identified that will help in identifying the biological behavior (when malignant lesions will be described), as well as the gene whose products could be potentially disease-specific targets for therapy.

Published

2004

10. Expression Profiling of Ameloblastic Carcinoma

Author

Carinci, Francesco, Palmieri, Annalisa, Delaiti, Gianfranco, Rubini, Corrado, Fioroni, Massimiliano, Martinelli, Marcella, Pezzetti, Furio, Scapoli, Luca, and Piattelli, Adriano

Abstract

Ameloblastic carcinoma (AC) is a malignant epithelial odontogenic tumor that histologically retains the features of ameloblastic differentiation and exhibits cytological features of malignancy in the primary or recurrent tumor. It may develop within a preexisting ameloblastoma or arise de novo or from an odontogenic cyst. Expression profiling by DNA microarray is a new molecular technology that allows the analysis of cell and tissue gene expression. By using DNA microarrays containing 19,200 genes, several genes whose expression was significantly upregulated or downregulated were identified in a case of AC. The differentially expressed genes cover a broad range of functional activities 1) transcription, 2) signaling transduction, 3) cell cycle regulation, 4) apoptosis control, and 5) differentiation. The data reported are, to our knowledge, the first genetic portrait of an AC. No final conclusion can be drawn; however, this portrait will be useful in investigating the biological behavior and in identifying possible gene targets for cancer therapy when more cases of this rare tumor are reported and compared.

Published

2004

11. Recent Developments in Orofacial Cleft Genetics

Author

Carinci, Francesco, Pezzetti, Furio, Scapoli, Luca, Martinelli, Marcella, Avantaggiato, Anna, Carinci, Paolo, Padula, Ernesto, Baciliero, Ugo, Gombos, Fernando, Laino, Gregorio, Rullo, Rosario, Cenzi, Roberto, Carls, Fredrick, and Tognon, Mauro

Abstract

Nonsyndromic cleft of the lip and/or palate (CLP or orofacial cleft) derives from an embryopathy with consequent failure of the nasal process and/or palatal shelves fusion. This severe birth defect is one of the most common malformations among live births. Nonsyndromic CLP is composed of two separate entities cleft lip and palate (CL±P) and cleft palate only (CPO). Both have a genetic background, and environmental factors probably disclose these malformations. In CL±P, several loci have been identified, and, in one case, a specific gene has also been found. In CPO, one gene has been identified, but many more are probably involved. Because of the complexity of the genetics of nonsyndromic CLP as a result of the difference between CL±P and CPO, heterogeneity of each group caused by the number of involved genes, type of inheritance, and interaction with environmental factors, we discuss the more sound results obtained with different approaches epidemiological studies, animal models, human genetic studies, and in vitro studies.

Published

2003

12. Expression Profiles of Craniosynostosis-Derived Fibroblasts

Author

Carinci, Francesco, Bodo, Maria, Tosi, Lara, Francioso, Francesca, Evangelisti, Rita, Pezzetti, Furio, Scapoli, Luca, Martinelli, Marcella, Baroni, Tiziano, Stabellini, Giordano, Carinci, Paolo, Bellucci, Catia, Lilli, Cinzia, and Volinia, Stefano

Abstract

Background: Craniosynostosis syndromes, a group of connective disorders characterized by abnormalities in vault osteogenesis and premature fusion of bone sutures, are associated with point mutations in FGF receptor family members. The cellular phenotype is characterized by abnormal extracellular matrix turnover. Material and Methods: We used primary cultures of periosteal fibroblasts derived from two different craniosynostosis syndromes, the Apert and Crouzon syndromes. The FGFR2 third immunoglobulin-like domain and its flanking linker regions were analyzed for mutation. DNA microarrays containing 19,200 cDNAs were used to study the gene expression profiles of Apert and Crouzon fibroblasts. The pathologic cells were compared to wild-type human periosteal fibroblasts. Results: The P253R missense mutation and the G338R mutation were observed in Apert and Crouzon fibroblasts, respectively. The genetic profiles, as evaluated by DNA microarrays, yielded different clusters of expressed sequence tag (ESTs) expression within the experiment. Expression profiles from craniosynostosis-derived fibroblasts differ from those of wild-type fibroblasts (288 human ESTs, p&lt; 0.01, pFDR = 0.12). Furthermore, two ESTs clusters discriminate the Crouzon from Apert fibroblasts. The differentially expressed genes cover a broad range of functional activities, including (1)bone differentiation, (2)cell-cycle regulation, (3)apoptotic stimulation, and (4)signaling transduction, cytoskeleton, and vesicular transport. Conclusions: The transcriptional program of craniosynostosis fibroblasts differs from that of wild-type fibroblasts. Expression profiles of Crouzon and Apert fibroblasts can also be distinguished by two EST expression clusters, thus hinting at a different genetic background.

Published

2002

13. Basic Fibroblast Growth Factor: Effects on Matrix Remodeling, Receptor Expression, and Transduction Pathway in Human Periosteal Fibroblasts with FGFR2 Gene Mutation

Author

Bodo, Maria, Lilli, Cinzia, Aisa, Maria Cristina, Scapoli, Luca, Bellucci, Catia, Rinaldi, Eliana, Tosi, Lara, Baroni, Tiziano, Conte, Carmela, Bellocchio, Silvia, Carinci, Francesco, Stabellini, Giordano, and Carinci, Paolo

Abstract

The Crouzon syndrome, which is associated with fibroblast growth factor receptor (FGFR2) mutations, is characterized by premature fusion of cranial sutures. We used an in vitro model of cultured periosteal fibroblasts from normal subjects and from Crouzon patients with FGFR2 mutation. We analyzed the matrix turnover rate and the effects of adding FGF2 by evaluating fibronectin synthesis and the activity of some proteolytic enzymes. To assess the role of some FGF signaling molecules involved in FGFR2 regulation, we studied Grb2 tyrosine phosphorylation and the phosphotyrosine proteins associated with Grb2. The iodinate FGF binding assay was performed to quantify FGFR expression. Compared with normal fibroblasts, fibronectin synthesis was decreased in Crouzon fibroblasts, and protease activities in cells and medium were enhanced, suggesting that excess fibronectin catabolism is present. Differences were more marked when FGF2 was added. Very few phosphoproteins were visible in anti-Grb2 immunoprecipitations from Crouzon fibroblasts, which showed a significant increase in the number of high-affinity and low-affinity FGF2 receptors. These results suggest that the abnormal genotype and the Crouzon cellular phenotype are related. To compensate the low levels of tyrosine phosphorylation, Crouzon cells might increase the numbers of FGFR2, thus increasing the cell surface binding sites for FGF2.

Published

2002

14. Cyclosporin A and transforming growth factor modify the pattern of extracellular glycosaminoglycans without causing cytoskeletal changes in human gingival fibroblasts1

Author

Stabellini, Giordano, Carinci, Francesco, Luigi Bedani, Pier, Calastrini, Carla, de Mattei, Monica, Scapoli, Luca, Caruso, Angelo, Calvitti, Mario, and Locci, Paola

Abstract

Cyclosporin A is a powerful immunosuppressive drug that has had a major impact on transplant therapy. It apparently links to different enzymatic pathways, and affects multiple enzymatic systems. Transforming growth factor induces the deposition of glycosaminoglycans, proteoglycans, and collagen fibers in the extracellular matrix. The aim of this study of normal and hypertrophic human gingival fibroblast cultures was to evaluate the cytoskeletal and extracellular changes in glycosaminoglycan secretion due to the presence of cyclosporin A and transforming growth factor . The results showed that there is an increase in total and individual classes of extracellular glycosaminoglycans in the presence of cyclosporin A and transforming growth factor , but the action of the latter was significantly greater. Immunohistochemical analysis of the cytoskeleton did not reveal any morphological differences between treated and control cells. Our data suggest that the biochemical changes in the extracellular matrix are caused more by cytokine, and that cyclosporin A does not induce any morphological changes in fibroblast cultures derived from hypertrophic and normal gingiva.

Published

2002

15. The Region on 9p Associated with 46,XY Sex Reversal Contains Several Transcripts Expressed in the Urogenital System and a Novel Doublesex-Related Domain

Author

Ottolenghi, Chris, Veitia, Reiner, Quintana-Murci, Lluis, Torchard, Delphine, Scapoli, Luca, Souleyreau-Therville, Nicole, Beckmann, Jacques, Fellous, Marc, and McElreavey, Ken

Abstract

Deletions of 9p have been associated with 46,XY gonadal dysgenesis, and the smallest region of overlap has been mapped to the tip of chromosome 9. Two candidate genes (DMRT1and 2) have been found in the region. Despite intensive mutation searches, no mutations have been detected in these genes. To gain insights into the genomics of the region and to isolate other candidate genes for the phenotype, we have constructed a P1 artificial chromosome (PAC)/bacterial artificial chromosome (BAC) contig spanning over 500 kb and covering the consensus critical region. We have analyzed the expression pattern of several ESTs mapped or sublocalized within the framework of the contig. In addition, a sample shotgun sequencing of a PAC containing the mentioned DM genes led to the detection of novel transcripts displaying an expression pattern specific to testis and kidney, consistent with a role in the development of the urogenital system. One of them, expressed in adult testis and human embryos aged 4–5 weeks, encodes a potential polypeptide and is located immediately downstream of a sequence capable of encoding a novel DM domain. The region was partially screened for mutations in sex-reversed patients by Southern blot, sequencing, and FISH. No mutations were found. Our results suggest that the critical region on 9p involved in male-to-female sex reversal displays greater gene density and genomic complexity than previously anticipated. Future investigations will include functional and mutational studies of the novel transcripts mapped or sublocalized within the critical region by this study as well as cloning efforts to isolate additional candidate genes.

Published

2000

16. Genetics of Nonsyndromic Cleft Lip and Palate: A Review of International Studies and Data regarding the Italian Population

Author

Carinci, Francesco, Pezzetti, Furio, Scapoli, Luca, Martinelli, Marcella, Carinci, Paolo, and Tognon, Mauro

Abstract

The aims of this review are (1) to illustrate current knowledge of the mode of inheritance and the loci involved in the cleft lip and palate and (2) to summarize the results of our investigations, which were carried out in Italy. It is well established that nonsyndromic cleft of the lip with or without the palate (CL±P) and cleft palate only (CPO) are separate entities. Genetic heterogeneity has been observed in CL±P, which involves different chromosome regions, mainly 6p23 (OFC1), 2q13 (OFC2), and 19q13.2 (OFC3), as well as other loci, such as 4q25-4q31.3 and 17q21. Furthermore, an interaction between different genes has been suggested in the oligogenic model. In one case at least, an OFC1 and OFC2 interaction has been demonstrated.The mode of inheritance of CPO is compatible with a recessive single major gene model, while an association with a candidate gene, mapping on the chromosome region 2q13/TGF a, remains to be confirmed.

Published

2000

17. Evidence of Linkage to 6p23 and Genetic Heterogeneity in Nonsyndromic Cleft Lip with or without Cleft Palate

Author

Scapoli, Luca, Pezzetti, Furio, Carinci, Francesco, Martinelli, Marcella, Carinci, Paolo, and Tognon, Mauro

Abstract

Nonsyndromic cleft lip with or without cleft palate (CL±P) is a congenital orofacial anomaly that derives from an embryopathy with failure of nasal process and palatal shelves fusion. CL±P is one of the most common malformations, affecting 1/700–1/1000 live births among Caucasians. Early investigations have suggested that a clefting gene may be located on the short arm of chromosome 6 (6p), as well as in other regions. In this study, we analyzed a large sample of families by using eight PCR markers that map on chromosome region 6p23–p24. The admixture test, as implemented in the HOMOG program, was significant when tested against multipoint data (α = 0.60,Pvalue 0.00004); the lod score calculated, assuming heterogeneity, was 3.60 at 1 cM telomeric to D6S259. Taken together these data demonstrate the presence of a locus for CL±P in the 6p23 chromosome region.

Published

1997

18. Lack of linkage disequilibrium between transforming growth factor alpha Taq I polymorphism and cleft lip with or without cleft palate in families from Northeastern Italy

Author

Scapoli, Luca, Pezzetti, Furio, Carinci, Francesco, Martinelli, Marcella, and Carinci, Paolo

Abstract

Cleft lip with or without cleft palate (CL ± P) is the most frequent craniofacial malformation in different human populations and its cause is largely unknown. Several studies based on population associations have suggested that an allele mapping in the transforming growth factor alpha locus could be responsible, as a risk factor, for the development of the defect. Our investigation of the Taq I polymorphism at the transforming growth factor alpha locus, performed in 40 CL ± P families, did not find evidence for linkage disequilibrium with particular alleles. Moreover, tight linkage was excluded with the traditional LOD score method. Am. J. Med. Genet. 75:203–206, 1998. © 1998 Wiley-Liss, Inc.

Published

1998

19. A Locus in 2p13–p14 (OFC2), in Addition to That Mapped in 6p23, Is Involved in Nonsyndromic Familial Orofacial Cleft Malformation

Author

Pezzetti, Furio, Scapoli, Luca, Martinelli, Marcella, Carinci, Francesco, Bodo, Maria, Carinci, Paolo, and Tognon, Mauro

Abstract

An allelic association between the transforming growth factor α gene (TGFA) situated in the chromosome 2p13 region and nonsyndromic cleft lip with or without cleft palate, also named orofacial cleft (OFC), was found in several population studies. However, no linkage between gene and malformation has shown up until now, probably due to the presence of genetic heterogeneity and the small sample size analyzed. Previously, we employed a collection of 38 OFC families to demonstrate linkage to the 6p23 chromosome region with the presence of genetic heterogeneity. In the present study we tested whether, in the same sample, linkage between OFC and markers on 2p13 could be determined. Evidence for genetic heterogeneity in our family set was apparent, by both pairwise and multipoint linkage analyses. Moreover, lod scores >3 were found for marker D2S378 when families linked to the 6p23 markers were analyzed. Taken together these results indicate a role for the TGFA, or for another gene physically close to it, and suggest an interaction between two different genes, OFC1 and OFC2, mapped in 6p23 and 2p13, respectively, in the development of the cleft.

Published

1998

20. Suggestive Linkage between Markers on Chromosome 19q13.2 and Nonsyndromic Orofacial Cleft Malformation

Author

Martinelli, Marcella, Scapoli, Luca, Pezzetti, Furio, Carinci, Francesco, Carinci, Paolo, Baciliero, Ugo, Padula, Ernesto, and Tognon, Mauro

Abstract

Nonsyndromic cleft lip with or without cleft palate (OFC) is a common birth defect that has genetic bases. The nature of the genetic contribution is still to be clarified; however, some chromosome regions and candidate genes have been proposed for this malformation. We examined linkage between BCL3, a proto-oncogene located in 19q13.2, and OFC in a sample composed of 40 multiplex pedigrees using both nonparametric and parametric methods. The affected pedigree member statistics and the transmission disequilibrium test supported a role for BCL3 in causing OFC, while no evidence of linkage or genetic heterogeneity was found with the lod score method.

Published

1998

21. Study of folate receptor genes in nonsyndromic familial and sporadic cleft lip with or without clef palate cases

Author

Scapoli, Luca, Marchesini, Jlenia, Martinelli, Marcella, Pezzetti, Furio, Carinci, Francesco, Palmieri, Annalisa, Rullo, Rosario, Gombos, Fernando, Tognon, Mauro, and Carinci, Paolo

Abstract

Folate receptor family members (FOLRs) mediate the delivery of 5‐methyltetrahydrofolate to the interior of, out of within, or between cells in a process known as potocytosis. Three FOLRsand a pseudogene map to 11q13.4. The aim of this study was to verify whether FOLRscould be responsible for the onset of nonsyndromic cleft lip with or without cleft palate (CL/P). Linkage and linkage disequilibrium between genetic markers and disorder were analyzed. Patients and their mothers from 71 familial CL/P pedigrees and 75 sporadic cases from Italian population were investigated by PCR‐SSCP analysis. Data from mutation scanning allowed us to find only a silent mutation in FOLR1present in a mother and her child. Our findings do not support FOLR1and FOLR2genes in the onset of CL/P. © 2004 Wiley‐Liss, Inc.

Published

2005

22. Spontaneous expression of FRA3P in a patient with Nager syndrome

Author

Scapoli, Luca, Martinelli, Marcella, Pezzetti, Furio, Carahelli, Elisabetta, Carinci, Francesco, Cenzi, Roberto, Meneghetti, Andrea, and Donti, Emilio

Abstract

No abstract

Published

2003

23. Berberine and Tinospora cordifoliaexert a potential anticancer effect on colon cancer cells by acting on specific pathways

Author

Palmieri, Annalisa, Scapoli, Luca, Iapichino, Anastasia, Mercolini, Laura, Mandrone, Manuela, Poli, Ferruccio, Giannì, Aldo Bruno, Baserga, Camilla, and Martinelli, Marcella

Abstract

Berberine (BBR) is a natural active principle with potential antitumor activity. The compound targets multiple cell signaling pathways, including proliferation, differentiation, and epithelial–mesenchymal transition. The aim of this study was to elucidate the mechanisms behind the anticancer activity of BBR by comparing the effects of purified BBR with those of the extract of Tinospora cordifolia, a medicinal plant that produces this metabolite. The expression levels of a panel of 44 selected genes in human colon adenocarcinoma (HCA-7) cell line were quantified by real-time polymerase chain reaction (PCR). BBR treatment resulted in a time- and dose-dependent down regulation of 33 genes differently involved in cell cycle, differentiation, and epithelial–mesenchymal transition. The trend was confirmed across the two types of treatment, the two time points, and the different absolute dosage of BBR. These findings suggest that the presence of BBR in T. cordifoliaextract significantly contributes to its antiproliferative activity.

Published

2019

24. Evaluation of IL6, IL10 and VDR alleles distribution in an Italian large sample of subjects affected by chronic periodontal disease

Author

Scapoli, Luca, Carinci, Francesco, Mucchi, Damiano, Nota, Alessandro, Caruso, Silvia, Rossi, Diego, Romano, Michele, and Severino, Marco

Abstract

In recent decades, the role played by the immune response to bacteria in the pathogenesis of chronic periodontal disease (PD) has long been studied. Although from the clinical point of view, adequate oral hygiene is essential to ensure a satisfactory response of the host to infections, modulation of the reaction of immune system could be influenced by genetic factors. The aim of the present study was to investigate the distribution of alleles of polymorphisms relevant for chronic periodontitis in a sample of adult subjects affected by chronic PD. The present study was conducted with sample collected in Italian private practice offices from January 2013 to December 2017. The sample included 744 adult patients diagnosed with chronic periodontitis. The inclusion criteria were as follows: age > 18 years, diagnosis of chronic PD. The diagnosis of chronic periodontitis was based on the criteria established by the American Academy of Periodontology. No significant difference in allele distribution among patients from different Italian regions was found. Results, supporting absence of population heterogeneity for the investigated polymorphisms in Italy, suggest similar effect in periodontitis etiology.

Published

2019

25. Gabapentin affects the expression of inflammatory mediators on healthy gingival cells

Author

Candotto, Valentina, Scapoli, Luca, Gaudio, Rosa Maria, Gianni, Aldo Bruno, Bolzoni, Alessandro, Racco, Pierpaolo, Lauritano, Dorina, and Cura, Francesca

Abstract

Gabapentin is one of the most used drugs to treat postoperative pain with antihyperalgesic properties and has a unique mechanism of action, which differentiates it from other commonly used drugs. Various studies have shown that the perioperative use of gabapentin reduces postoperative pain. In our study, fragments of gingival tissue of healthy volunteers were collected during operation. Gene expression of 29 genes was investigated in gingival fibroblasts cell culture treated with gabapentin, compared with untreated cells. Of the different chemokines and interleukins studied, only 10 were statistically significant (CCL1, CCR1, CCR4, CCR5, CCR6, ILI1A, ILI1B, IL5, IL6R, TNFSF10). The overexpression of these cytokines, obtained in many studies, leads us to think that gabapentin can interact and cause post-inflammatory gingival hyperplasia, but, probably, in our study the gabapentin has not the same effect, because we used gingival fibroblasts of healthy people.

Published

2019

26. Non-syndromic cleft palate: Association analysis on three gene polymorphisms of the folate pathway in Asian and Italian populations

Author

Carinci, Francesco, Palmieri, Annalisa, Scapoli, Luca, Cura, Francesca, Borelli, Francesco, Morselli, Paolo Giovanni, Nouri, Nayereh, Abdali, Hossein, Gianni, Aldo Bruno, Russillo, Antonio, Docimo, Raffaella, and Martinelli, Marcella

Abstract

Periconceptional folic acid supplementation can reduce the risk of inborn malformations, including orofacial clefts. Polymorphisms of MTHFR, TCN2, and CBS folate-related genes seem to modulate the risk of cleft lip with or without cleft palate (CL/P) in some populations. CL/P and cleft palate only (CPO) are different malformations that share several features and possibly etiological causes. In the present investigation, we conducted a family-based, candidate gene association study of non-syndromic CPO. Three single nucleotide polymorphisms, namely, rs1801133 of MTHFR, rs1801198 of TCN2, and rs4920037 of CBS, were investigated in a sample that included 129 Italian and 65 Asian families. No evidence of association between the three genotyped polymorphisms and CPO was found in the Italian and Asian cases, indeed the transmission disequilibrium test did not detect any asymmetry of transmission of alleles. This investigation, although with some limitation, further supports that CL/P and CPO diverge in their genetic background.

Published

2019

27. Copy number variation analysis of twin pairs discordant for cleft lip with or without cleft palate

Author

Scapoli, Luca, Carinci, Francesco, Palmieri, Annalisa, Cura, Francesca, Baj, Alessandro, Beltramini, Giada, Docimo, Raffaella, and Martinelli, Marcella

Abstract

Non-syndromic cleft lip with or without cleft palate (nsCL/P) is a frequent orofacial malformation. The comparison of concordance rate observed in monozygotic and dizygotic twins supports high level of heritability and a strong genetic component. However, phenotype concordance for orofacial cleft in monozygotic twins is about 50%. The aim of the present investigation was to detect postzygotic events that may account for discordance in monozygotic twins. High-density SNP microarrays hybridization was used to genotype two pairs of monozygotic twins discordant for nsCL/P. Discordant SNP genotypes and copy number variants were analyzed to identify genetic differences responsible of phenotype discrepancy. A number of differences were observed, none involving known nsCL/P candidate genes or genomic regions. Considering the limitation of the study, related to the small sample size and to the large-scale investigation method, the results suggest that the detection of discordant events in other monozygotic twin pairs would be remarkable and warrant further investigations.

Published

2019

28. Association between oral cleft and transcobalamin 2 polymorphism in a sample study from Nassiriya, Iraq

Author

Carinci, Francesco, Palmieri, Annalisa, Scapoli, Luca, Cura, Francesca, Abenavoli, Fabio, Giannì, Aldo Bruno, Russillo, Antonio, Docimo, Raffaella, and Martinelli, Marcella

Abstract

Orofacial clefts are common congenital defects whose prevalence differs between geographical regions and ethnic groups. The inheritance is complex, involving the contribution of both genetic and environmental factors. The involvement of genes belonging to the folate pathway is still matter of debate, with strong evidences of association and conflicting results. After demonstrating the contribution, for a sample from the Italian population, of common mutations mapping on three genes of the folate pathway, our group tried to unravel their contribution in independent sample studies with different ethnicity. In the present investigation a set of 34 triads with oral cleft from Nassiriya, Iraq, has been genotyped for rs1801133 of MTHFR, rs1801198 of TCN2, and rs4920037 of CBS polymorphisms. Association analysis evidenced a decreased risk of cleft for children carrying the 667G allele at TCN2 gene (P= 0.02). This evidence further supported the relationship between polymorphisms of folate related genes and oral clefts, and outlined the relevance of studying populations having different ethnicity.

Published

2019

29. Investigation of the W185X nonsense mutation of <TOGGLE>PVRL1</TOGGLE> gene in Italian nonsyndromic cleft lip and palate patients

Author

Scapoli, Luca, Marchesini, Jlenia, Palmieri, Annalisa, Carinci, Francesco, Pezzetti, Furio, Martinelli, Marcella, Gombos, Fernando, Delaiti, Gianfranco, Tognon, Mauro, and Carinci, Paolo

Abstract

No abstract

Published

2004