Fragile Histidine Triad Expression in Oral Squamous Cell Carcinoma and Precursor Lesions

Kujan, Omar; Oliver, Richard; Roz, Luca; Sozzi, Gabriella; Ribeiro, Noel F.F.; Woodwards, R.T.; Thakker, Nalin; Sloan, Philip

doi:10.1158/1078-0432.ccr-06-1475

Cited by 15 publications

(16 citation statements)

References 42 publications

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“…Characterization of the pattern of human FHIT expression could contribute to our understanding of the function of this protein in normal tissues and provide a reference framework for interpretation of abnormal FHIT expression in human tumors. In contrast to previously published studies that reported exclusively cytoplasmic localization of FHIT, we showed a nuclear and cytoplasmic localization of the FHIT protein by immunohistochemical methods [12]. We, therefore, aim to perform a comprehensive immunohistochemical analysis of FHIT expression in normal human tissues and compare FHIT expression with proliferation and diff erentiation within individual organs.…”

Section: Introductioncontrasting

confidence: 60%

“…For scoring, negative and low (no staining or immunoreactivity staining present in <10% of cells) staining scores and moderate (immunoreactivity in ≥10-50% of cells) and strong (immunoreactivity in >50% of cells) staining scores were combined as negative or positive, respectively, as described previously by Kujan et al [12]. The software SPSS 22.0 was used to analyze all the statistical analyses.…”

Section: Discussionmentioning

confidence: 99%

“…FHIT immunohistochemical testing was performed according to the protocol that was developed earlier by Kujan et al [12] using primary rabbit polyclonal anti-glutathione S-transferase-FHIT antibody (abcam, Cambridge, UK). Briefl y, three paraffi n-embedded, formalin-fi xed sections from each studied organ were deparaffi nized, rehydrated, and immersed in 0.5% H 2 O 2 -methanol for 5 min.…”

Section: Immunohistochemical Techniquementioning

confidence: 99%

“…The FHIT gene can be inactivated by several mechanisms, including deletions, point mutations, methylation, loss of a whole chromosome, and genetic recombination. It was reported that the loss or decreased RNA and protein products of FHIT was found in stomach, liver, cervix, esophagus, breast, renal, pulmonary, gall bladder, colon, and oral cavity tumors, as well as leukemia [5,11,12].…”

Section: Introductionmentioning

confidence: 99%

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Immunohistochemical characterization of FHIT expression in normal human tissues

Kujan

Abuderman

Al-Shawaf

2016

IMAS

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Abstract:Background: Fragile histidine triad (FHIT) is a tumor suppressor gene that is commonly inactivated in human tumors. Interestingly, the normal pattern of FHIT expression is largely unknown. Aim: This study is aimed to characterize the expression of FHIT protein in normal human tissues. Materials and methods: A total of 119 normal human tissue specimens were analyzed for the FHIT expression using immunohistochemistry technique. The inclusion criteria included: normal/infl ammatory tissue with no evidence of cellular atypia. Results: All studied specimens were stained positively with FHIT and showed either nuclear or cytoplasmic expression. Interestingly, the pattern of FHIT staining was similar among diff erent specimens from each organ. FHIT is located predominantly in the nucleus, although cytoplasmic staining is also present in some cell types. Oral squamous epithelium, breast ductal epithelium, squamous and tubal metaplastic epithelium of the uterine cervix, esophageal squamous epithelium, salivary glands, and bronchial epithelia all strongly expressed the nuclear protein. In connective tissue, FHIT has shown strong cytoplasmic expression in histocytes including macrophages and dendritic cells, fi broblasts, and myofi broblasts. Conclusion: Documentation of the pattern of FHIT expression in normal tissues will contribute to our understanding of the normal function of this protein and to interpretation of potentially altered FHIT expression in human tumors.

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Section: Introductioncontrasting

confidence: 60%

Section: Discussionmentioning

confidence: 99%

Section: Immunohistochemical Techniquementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Immunohistochemical characterization of FHIT expression in normal human tissues

Kujan

Abuderman

Al-Shawaf

2016

IMAS

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“…Few studies have identified FHIT to be a predictor of poor survival in OSCC [34] in HNSCC [35]. However, these studies did not analyze the status of p53 aberrations in the tumors.…”

Section: Discussionmentioning

confidence: 99%

P53 nuclear stabilization is associated with FHIT loss and younger age of onset in squamous cell carcinoma of oral tongue

et al. 2014

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BackgroundSquamous cell carcinoma of tongue (SCCT) is expected to harbor unique clinico-pathological and molecular genetic features since a significant proportion of patients are young and exhibit no association with tobacco or alcohol.MethodsWe determined P53, epidermal growth factor receptor, microsatellite instability, human papilloma virus infection and loss of heterozygosity status at several tumor suppressor loci in one hundred and twenty one oral SCCT (SSCOT) samples and analyzed their association with clinico-pathological features and patient survival.ResultsOur results revealed a significantly higher incidence of p53 nuclear stabilization in early (as against late) onset SCCOT. FHIT loss was significantly associated with p53 nuclear stabilization and the association was stronger in patients with no history of tobacco use. Samples harboring mutation in p53 DNA binding domain or exhibiting p53 nuclear stabilization, were significantly associated with poor survival.ConclusionOur study has therefore identified distinct features in SCCOT tumorigenesis with respect to age and tobacco exposure and revealed possible prognostic utility of p53.

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Fhit Nuclear Import Following EGF Stimulation Sustains Proliferation of Breast Cancer Cells

Bianchi

Sasso

Turdo

et al. 2015

Journal Cellular Physiology

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The tumor-suppressor protein fragile histidine triad (Fhit) exerts its functions in the cytoplasm, although some reports suggest that it may also act in the nucleus. We previously showed that cytosolic Fhit protein levels in cancer cell lines stimulated to proliferate were reduced by proteasomal degradation. Here, we demonstrate that Fhit is physiologically present in the nucleus of breast cancer cell lines and tissues at a low level and that proliferative stimulation increases nuclear levels. Breast cancer cells expressing the FhitY114F mutant, which do not undergo proteasomal degradation, contained mutated Fhit in the nucleus, while cells treated with a proteasome inhibitor accumulated nuclear Fhit during proliferation. Thus, Fhit nuclear shuttling and proteasome degradation phenomena occur independently. When Fhit was coupled to a nuclear localization sequence, the proliferation rate of the transfected cells increased together with levels of proliferation pathway mediators cyclin D1, phospho-MAPK, and phospho-STAT3. Fhit nuclear translocation upon mitogenic stimulation may represent a new regulatory mechanism that allows rapid restoration of Fhit cytoplasmic levels and promotes the proliferation cascade activated by mitogenic stimulation.

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Fragile Histidine Triad Expression in Oral Squamous Cell Carcinoma and Precursor Lesions

Cited by 15 publications

References 42 publications

Immunohistochemical characterization of FHIT expression in normal human tissues

Immunohistochemical characterization of FHIT expression in normal human tissues

P53 nuclear stabilization is associated with FHIT loss and younger age of onset in squamous cell carcinoma of oral tongue

Fhit Nuclear Import Following EGF Stimulation Sustains Proliferation of Breast Cancer Cells

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