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17 results on '"Ekalaksananan, Tipaya"'

3. The Inhibitory Effect of Kerra TM , KS TM , and Minoza TM on Human Papillomavirus Infection and Cervical Cancer.

Author

Choowongkomon, Kiattawee, Choengpanya, Khuanjarat, Pientong, Chamsai, Ekalaksananan, Tipaya, Talawat, Sulak, Srathong, Pussadee, and Chuerduangphui, Jureeporn

Subjects
HUMAN papillomavirus, PAPILLOMAVIRUS diseases, CERVICAL cancer, HELA cells, CELL populations
Abstract

Background and Objectives: Cervical cancer is one of the most common types of frequently found cancers in Thailand. One of the causative agents is the infection of the high-risk human papillomavirus (HPV) type 16 and 18. Traditional medicines are rich sources of bioactive compounds which are a valuable source for the development of novel cancer therapies. In this study, the therapeutic effects of 3 traditional medicines, KerraTM, KSTM, and MinozaTM, were studied on HeLa and CaSki cells. Materials and Methods: The effects of KerraTM, KSTM, and MinozaTM on cancer cells were evaluated through cytotoxicity and cell death assays. The infection assay using HPV-16 pseudovirus was also carried out. Results: All traditional medicines efficiently suppressed cell growths of HeLa and CaSki, with KerraTM being the most potent anticancer agent followed by KSTM and MinozaTM. KerraTM at 158 µg/mL and 261 µg/mL significantly increases the percentage inhibition of the HPV-16 pseudovirus infection in a pre-attachment step in a dose-dependent manner, while KSTM at 261 µg/mL efficiently inhibited viral infection in both pre-attachment and adsorption steps. However, KerraTM, KSTM, and MinozaTM at subtoxic concentrations could not reduce the viral E6 mRNA expressions of HPV-16 and HPV-18. Cell death assay by acridine orange/ethidium bromide showed that KerraTM increased population of dead cells in dose-dependent manner in both CaSki and HeLa. The percentage of secondary necrosis in KerraTM-treated CaSki was higher than that of HeLa cells, while the percentage of late apoptotic cells in HeLa was higher than that of CaSki, indicating that HeLa was more susceptible to KerraTM than CaSki. For KSTM and MinozaTM, these extracts at 250 µg/mL promoted autophagy over cell death. At 500 µg/mL, the percentage of dead cells in KerraTM was higher than that of KSTM and MinozaTM. Conclusions: KerraTM is a potent traditional medicine for promoting cancer cell death. KerraTM is possibly useful in the prevention and treatment of cervical cancer. Further investigation will be carried out to gain a better understanding of the biochemical mechanism and the pharmacological activity underlying this effect. [ABSTRACT FROM AUTHOR]

Published
2023
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7. Epidemiological evidence and association of human papillomavirus with esophageal cancer in northeastern Thailand: a case--control study.

Author

Burassakarn, Ati, Pientong, Chamsai, Tongchai, Panwad, Wongjampa, Weerayut, Poosari, Arisara, Udomsin, Apiradee, Sa-ngiamwibool, Prakasit, Ungareewittaya, Piti, Nutravong, Thitima, and Ekalaksananan, Tipaya

Subjects
HUMAN papillomavirus, ESOPHAGEAL cancer, PAPILLOMAVIRUSES, GASTROESOPHAGEAL reflux, DISEASE risk factors, PUBLICATION bias
Abstract

Recently, epidemiological evidence of high-risk human papillomavirus (hrHPV) and its association with the increasing risk of esophageal cancer (EC) have been described. However, the involvement of such a virus in the pathogenesis of EC is still inconclusive in the literature. Therefore, our objective was to clarify the epidemiology of HPV infections in primarily diagnosed EC cases and validate this correlation with hospital-based control patients using a retrospective study with a case--control model. Here, we reported that the overall prevalence of HPV DNA was statistically associated with an increased risk of EC (OR, 3.3; 95% CI, 2.5--4.3). Interestingly, a history of gastroesophageal reflux disease (GERD) was constituted and significantly associated with HPV prevalence (adjusted OR, 4.6; 95% CI, 2.2--9.5). Furthermore, our meta-analysis in public databases also indicated that the combined OR and 95% CI between HPV infection and EC risk were 3.31 and 2.53--4.34, respectively, with significant heterogeneity (I2 =78%). Variations in the geographic study, tissue type, and detection method remain potential predictors of heterogeneity. In addition, publication bias and sensitivity analysis were not observed, and the results exhibited stable outcomes. Collectively, we specify the recent epidemiological evidence in a validation of the distributed HPV, which might be statistically associated with an increased risk of EC. However, additional high-quality studies with larger sample sizes are needed to further verify the link between HPV and EC. [ABSTRACT FROM AUTHOR]

Published
2023
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8. Mathematical Modelling of Cervical Precancerous Lesion Grade Risk Scores: Linear Regression Analysis of Cellular Protein Biomarkers and Human Papillomavirus E6 / E7 RNA Staining Patterns.

Author

Bumrungthai, Sureewan, Ekalaksananan, Tipaya, Kleebkaow, Pilaiwan, Pongsawatkul, Khajohnsilp, Phatnithikul, Pisit, Jaikan, Jirad, Raumsuk, Puntanee, Duangjit, Sureewan, Chuenchai, Datchani, and Pientong, Chamsai

Subjects
*DISEASE risk factors, *HUMAN papillomavirus, *PRECANCEROUS conditions, *REGRESSION analysis, *CELL analysis, *P16 gene
Abstract

The current practice of determining histologic grade with a single molecular biomarker can facilitate differential diagnosis but cannot predict the risk of lesion progression. Cancer is caused by complex mechanisms, and no single biomarker can both make accurate diagnoses and predict progression risk. Modelling using multiple biomarkers can be used to derive scores for risk prediction. Mathematical models (MMs) may be capable of making predictions from biomarker data. Therefore, this study aimed to develop MM–based scores for predicting the risk of precancerous cervical lesion progression and identifying precancerous lesions in patients in northern Thailand by evaluating the expression of multiple biomarkers. The MMs (Models 1–5) were developed in the test sample set based on patient age range (five categories) and biomarker levels (cortactin, p16INK4A, and Ki–67 by immunohistochemistry [IHC], and HPV E6/E7 ribonucleic acid (RNA) by in situ hybridization [ISH]). The risk scores for the prediction of cervical lesion progression ("risk biomolecules") ranged from 2.56–2.60 in the normal and low–grade squamous intraepithelial lesion (LSIL) cases and from 3.54–3.62 in cases where precancerous lesions were predicted to progress. In Model 4, 23/86 (26.7%) normal and LSIL cases had biomolecule levels that suggested a risk of progression, while 5/86 (5.8%) cases were identified as precancerous lesions. Additionally, histologic grading with a single molecular biomarker did not identify 23 cases with risk, preventing close patient monitoring. These results suggest that biomarker level–based risk scores are useful for predicting the risk of cervical lesion progression and identifying precancerous lesion development. This multiple biomarker–based strategy may ultimately have utility for predicting cancer progression in other contexts. [ABSTRACT FROM AUTHOR]

Published
2023
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9. An in vitro carcinogenesis model for cervical cancer harboring episomal form of HPV16.

Author

Wongjampa, Weerayut, Nakahara, Tomomi, Tanaka, Katsuyuki, Yugawa, Takashi, Ekalaksananan, Tipaya, Kleebkaow, Pilaiwan, Goshima, Naoki, Kiyono, Tohru, and Pientong, Chamsai

Subjects
CERVICAL cancer, GENE expression, ONCOGENES, VIRAL genomes, HUMAN papillomavirus, CARCINOGENESIS, HELA cells
Abstract

Deregulated expression of viral E6 and E7 genes often caused by viral genome integration of high-risk human papillomaviruses (HR-HPVs) into host DNA and additional host genetic alterations are thought to be required for the development of cervical cancer. However, approximately 15% of invasive cervical cancer specimens contain only episomal HPV genomes. In this study, we investigated the tumorigenic potential of human cervical keratinocytes harboring only the episomal form of HPV16 (HCK1T/16epi). We found that the HPV16 episomal form is sufficient for promoting cell proliferation and colony formation of parental HCK1T cells. Ectopic expression of host oncogenes, MYC and PIK3CAE545K, enhanced clonogenic growth of both early- and late-passage HCK1T/16epi cells, but conferred tumor-initiating ability only to late-passage HCK1T/16epi cells. Interestingly, the expression levels of E6 and E7 were rather lower in late-passage than in early-passage cells. Moreover, additional introduction of a constitutively active MEK1 (MEK1DD) and/or KRASG12V into HCK1T/16epi cells resulted in generation of highly potent tumor-initiating cells. Thus an in vitro model for progression of cervical neoplasia with episomal HPV16 was established. In the model, constitutively active mutation of PIK3CA, PIK3CAE545K, and overexpression of MYC, in the cells with episomal HPV16 genome were not sufficient, but an additional event such as activation of the RAS-MEK pathway was required for progression to tumorigenicity. [ABSTRACT FROM AUTHOR]

Published
2023
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10. Prevalence of human papillomavirus in oral rinse samples from healthy individuals in northern Thailand.

Author

Bumrungthai, Sureewan, Ekalaksananan, Tipaya, Duangchai, Darin, Lanpol, Pornsiri, Panya, Papichaya, Kattiwong, Fernladda, Acharya, Sulav, and Pientong, Chamsai

Subjects
*DISEASE prevalence, *PAPILLOMAVIRUSES, *SALIVA analysis, *GENOTYPES, *POLYMERASE chain reaction, *NUCLEOTIDE sequencing, *HEALTH risk assessment
Abstract

Background: The incidence of oral cancers associated with human papillomavirus (HPV) has been increasing in recent years. Therefore, it is necessary to elucidate HPV prevalence in oral cells and exposure to risk factors in various age groups.Methods: Oral rinse samples from healthy individuals in northern Thailand were investigated for HPV prevalence and genotyped using the polymerase chain reaction (GP5+/6+ primers) and DNA sequencing of the PCR products.Results: Samples were collected from 594 participants between 4 and 60 years of age. HPV was detected in 3.7% of samples. The prevalence of HPV-positive cases was 8.6% in the 31-50 age group. HPV prevalence increased with age and was the highest (9.2%) in the 41-50 age group, but decreased (to 3%) in the 51-60 age group. Risk factors significantly associated with HPV-positive cases included alcohol consumption, coffee drinking, sexual activity, and having children. HPV 16 and 18 were common genotypes, especially in the 31-50 age group, and were associated with having sexual activity (odds ratio 19.0 [95% CI: 2.5-142.5]). At follow-up of some individuals in the 4-10 age group, a 9-year-old child was found to be positive for HPV18.Conclusions: These results suggest that HPV can be acquired at a young age and the prevalence peaks in the middle age class among healthy individuals in northern Thailand, especially in the 31-50 age group. [ABSTRACT FROM AUTHOR]

Published
2019
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11. Human papillomavirus (HPV) infection in a case-control study of oral squamous cell carcinoma and its increasing trend in northeastern Thailand.

Author

Phusingha, Pensiri, Ekalaksananan, Tipaya, Vatanasapt, Patravoot, Loyha, Kulchaya, Promthet, Supannee, Kongyingyoes, Bunkerd, Patarapadungkit, Natcha, Chuerduangphui, Jureeporn, and Pientong, Chamsai

Abstract

Human papillomavirus (HPV) is an independent risk factor for development of oral squamous cell carcinoma (OSCC). This study aimed to investigate the role of HPV infection and the trend in percentage of HPV-associated OSCC over a 5-year period in northeastern Thailand. In this case-control study, 91 exfoliated oral cell samples and 80 lesion cell samples from OSCC cases and exfoliated oral cells from 100 age/gender-matched controls were collected. HPV infection was investigated by PCR using GP5+/GP6+ primers followed by HPV genotyping using reverse line blot hybridization. Quantitative RT-PCR was used to evaluate HPV oncogene transcription. Temporal trends of HPV infection were evaluated in archived formalin-fixed paraffin-embedded (FFPE) OSCC tissues using in situ hybridization. HPV DNA was found in 17.5% (14/80) of lesion samples from OSCC cases and 29.7% (27/91) of exfoliated oral cell samples from the same cases. These values were significantly higher than in exfoliated oral cell samples from controls (13%, 13/100). HPV-16 was the genotype most frequently found in OSCC cases (92.8%, 13/14 infected cases). Interestingly, HPV oncogene mRNA expression was detected and correlated with OSCC cases ( P < 0.005). Of 146 archived FFPE OSCC samples, 82 (56.2%) were positive for high-risk HPV DNA and 64 (43.8%) cases were positive for HPV E6/E7 mRNA expression. There was a trend of increasing percentage of HPV-associated OSCC from 2005 to 2010. This was especially so for females with well-differentiated tumors in specific tongue sub-sites. We suggest that HPV infection plays an important role in oral carcinogenesis in northeastern Thailand. [ABSTRACT FROM AUTHOR]

Published
2017
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12. The Three Most Common Human Papillomavirus Oncogenic Types and Their Integration State in Thai Women with Cervical Precancerous Lesions and Carcinomas.

Author

Aromseree, Sirinart, Chaiwongkot, Arkom, Ekalaksananan, Tipaya, Kongyingyoes, Bunkerd, Patarapadungkit, Natcha, and Pientong, Chamsai

Abstract

To understand the potential role in cervical cancer development of the three most common high-risk human papillomavirus (HRHPVs) in Thai women, HPV genotypes and viral genome statuses in different cervical lesions were investigated. Cervical tissues consisting of no cervical intraepithelial neoplasia (84 cases), grade I cervical intraepithelial neoplasia (176 cases), grade II-III cervical intraepithelial neoplasia (91 cases), and squamous cell carcinoma (66 cases) were subjected for HPV genotyping by polymerase chain reaction (PCR) and reverse line blot hybridization assay and for HPV genome status determination by amplification of papillomavirus oncogene transcripts (APOT) assay. HPV prevalence was 28.6% in no cervical intraepithelial neoplasia, 40.3% in grade I cervical intraepithelial neoplasia, 70.3% in grade II-III cervical intraepithelial neoplasia and 86.4% in squamous cell carcinoma cases. The three most common HR-HPV types were HPV 16, 58, and 18 which were distributed in all cervical lesions. HPV physical statuses could be investigated in 4 no cervical intraepithelial neoplasias, 2 grade I cervical intraepithelial neoplasias, 28 grade II-III cervical intraepithelial neoplasias and 31 squamous cell carcinomas. The integrated-derived transcripts were found 3.6% in grade II-III cervical intraepithelial neoplasia and 48.4% in squamous cell carcinoma, whereas no viral genome integration was found in the group of no cervical intraepithelial neoplasia or grade I cervical intraepithelial neoplasia samples. The frequencies of HR-HPV integration in squamous cell carcinoma were found 40%, 100%, 20% of HPV 16, 18, and 58. This study indicates the oncogenic potential ability of the three most common HR-HPVs associated with cervical cancer progression [ABSTRACT FROM AUTHOR]

Published
2014
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13. Differential methylation of E2 binding sites in episomal and integrated HPV 16 genomes in preinvasive and invasive cervical lesions.

Author

Chaiwongkot, Arkom, Vinokurova, Svetlana, Pientong, Chamsai, Ekalaksananan, Tipaya, Kongyingyoes, Bunkerd, Kleebkaow, Pilaiwan, Chumworathayi, Bandit, Patarapadungkit, Natcha, Reuschenbach, Miriam, and von Knebel Doeberitz, Magnus

Abstract

Enhanced expression of the HPV 16 E6-E7 oncogenes may trigger neoplastic transformation of the squamous epithelial cells at the uterine cervix. The HPV E2 protein is a key transcriptional regulator of the E6-E7 genes. It binds to four E2 binding sites (E2BSs 1-4) in the viral upstream regulatory region (URR). Modification of E2 functions, for example, by methylation of E2BSs is hypothesized to trigger enhanced expression of the viral E6-E7 oncogenes. In the majority of HPV-transformed premalignant lesions and about half of cervical carcinomas HPV genomes persist in an extra-chromosomal, episomal state, whereas they are integrated into host cells chromosomes in the remaining lesions. Here we compared the methylation profile of E2BSs 1-4 of the HPV 16 URR in a series of 18 HPV16-positive premalignant lesions and 33 invasive cervical cancers. CpGs within the E2BSs 1, 3, and 4 were higher methylated in all lesions with only episomal HPV16 genomes compared with lesions displaying single integrated copies. Samples with multiple HPV16 integrated copies displayed high methylation levels for all CpGs suggesting that the majority of multiple copies were silenced by extensive methylation. These data support the hypothesis that differential methylation of the E2BSs 1, 3 and 4 is related to the activation of viral oncogene expression in cervical lesions as long as the viral genome remains in the episomal state. Once the virus becomes integrated into host cell chromosomes these methylation patterns may be substantially altered due to complex epigenetic changes of integrated HPV genomes. [ABSTRACT FROM AUTHOR]

Published
2013
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14. Association of antibody to E2 protein of human papillomavirus and p16INK4A with progression of HPV-infected cervical lesions.

Author

Chuerduangphui, Jureeporn, Pientong, Chamsai, Swangphon, Piyawut, Luanratanakorn, Sanguanchoke, Sangkomkamhang, Ussanee, Tungsiriwattana, Thumwadee, Kleebkaow, Pilaiwan, Burassakarn, Ati, and Ekalaksananan, Tipaya

Abstract

Human papillomavirus (HPV) E2 and L1 proteins are expressed in cervical cells during the lytic stage of infection. Overexpression of p16INK4A is a biomarker of HPV-associated cervical neoplasia. This study investigated antibodies to HPV16 E2, HPV16 L1, and p16INK4A in sera from women with no squamous intraepithelial lesion (No-SIL) of the cervix, low-grade SIL, high-grade SIL, and cervical squamous cell carcinoma (SCC). HPV DNA was detected by polymerase chain reaction. Anti-E2, -L1, and -p16INK4A antibodies in sera were determined by western blot. Among 116 samples, 69 (60%) were HPV DNA-positive. Percentages seropositive for anti-E2, -L1, and -p16INK4A antibodies were 39.6, 22.4, and 23.3%, respectively. Anti-E2 antibody was significantly correlated with HPV DNA-positive cases. Eighty-seven women (75%) were regarded as infected with HPV, having at least one positive result from HPV DNA, L1, or E2 antibody. Antibody to p16INK4A was associated with HPV infection (odds = 5.444, 95% CI 1.203-24.629, P = 0.028) and precancerous cervical lesions (odds = 5.132, 95% CI 1.604-16.415, P = 0.006). Interestingly, the concurrent detection of anti-E2 and -p16INK4A antibodies was significantly associated with HPV infection (odds = 1.382, 95% CI 1.228-1.555, P = 0.044). These antibodies might be good candidate biomarkers for monitoring HPV-associated cervical lesion development to cancer. [ABSTRACT FROM AUTHOR]

Published
2018
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15. Peroxiredoxin-2 and zinc-alpha-2-glycoprotein as potentially combined novel salivary biomarkers for early detection of oral squamous cell carcinoma using proteomic approaches.

Author

Heawchaiyaphum, Chukkris, Pientong, Chamsai, Phusingha, Pensiri, Vatanasapt, Patravoot, Promthet, Supannee, Daduang, Jureerut, Teeramatwanich, Watchareporn, Kongyingyoes, Bunkerd, Chuerduangphui, Jureeporn, and Ekalaksananan, Tipaya

Subjects
*PEROXIREDOXINS, *GLYCOPROTEINS, *TUMOR markers, *SQUAMOUS cell carcinoma, *PROTEOMICS, *DIAGNOSIS
Abstract

No effective screening method is available for oral squamous cell carcinoma (OSCC) that is recognized to influence by environmental factors as well as human papillomavirus (HPV) and Epstein-Barr virus (EBV). Therefore, we sought to identify salivary biomarkers for screening of OSCC with or without HPV and/or EBV infection. Saliva, lesion and oral exfoliated cells were collected from OSCC patients and cancer-free controls (CFCs) and grouped depending on their HPV- and EBV-infection status. Salivary protein was precipitated and subjected to 2-dimensional gel electrophoresis. Differential expression of proteins was identified by mass spectrometry and validated by Western blotting. Distinctive expression patterns of salivary proteins were detected in OSCC as compared with CFCs. Levels of peroxiredoxin-2 (PRDX-2) and zinc-alpha-2-glycoprotein (ZAG) were significantly up-regulated in OSCC cases (p < 0.001) relative to CFCs. Similarly, these proteins were also up-regulated in lesion cells compared with oral exfoliated cells (p < 0.001). However, the expression patterns of these proteins were not significantly influenced by patient histories (risk factors). In combination, these proteins yielded the highest discriminatory power (AUC = 0.999), sensitivity (100%), and specificity (98.77%) in distinguishing the early stages of OSCC. The detection of PRDX-2 combining with ZAG protein could potentially be used as salivary biomarkers for early screening of OSCC. Significance Our findings demonstrate a useful of combined detection of PRDX-2 and ZAG as a salivary biomarker for the early detection of OSCC. [ABSTRACT FROM AUTHOR]

Published
2018
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16. Possible contributing role of Epstein-Barr virus (EBV) as a cofactor in human papillomavirus (HPV)-associated cervical carcinogenesis.

Author

Aromseree, Sirinart, Pientong, Chamsai, Swangphon, Piyawut, Chaiwongkot, Arkom, Patarapadungkit, Natcha, Kleebkaow, Pilaiwan, Tungsiriwattana, Thumwadee, Kongyingyoes, Bunkerd, Vendrig, Tineke, Middeldorp, Jaap M., and Ekalaksananan, Tipaya

Subjects
*EPSTEIN-Barr virus diseases, *COFACTORS (Biochemistry), *PAPILLOMAVIRUS diseases, *CERVICAL cancer treatment, *CARCINOGENESIS, *FORMALDEHYDE
Abstract

Background Persistent infection with EBV has been linked to the development of malignancies including HPV-associated cervical carcinoma. However, the role of EBV in HPV-associated cervical cancer is still poorly understood. Objective To determine the possible contributing role of EBV in HPV-associated cervical carcinogenesis according to HPV genotypes, HPV genome status and EBV localization. Study design Cervical tissues, including 82 with no squamous intraepithelial lesions (noSILs), 85 low-grade SILs (LSILs), 85 high grade SILs (HSILs) and 40 squamous cell carcinoma samples (SCC) were investigated using PCR and dot blot hybridization for EBV detection and PCR and reverse line blot hybridization for HPV genotyping. The amplification of papillomavirus oncogene transcripts assay and in situ hybridization were used to determine HPV physical status and EBV EBER localization, respectively. Results EBV was detected increasingly from noSIL (13.4%), LSIL (29.4%) to HSIL (49.4%) samples. The prevalence of HPV–EBV co-infection was significantly higher in any grade of lesion than in noSIL samples ( p < 0.05) including noSIL (1.2%; 95% confidence intervals [CI] = 0.0–3.6%, relative risk [RR] = 1), LSIL (18.8%, 95% CI = 10.5–27.1%, RR = 15.4), HSIL (41.2%, 95% CI = 30.7–51.6%, RR = 33.8) and SCC (30.0%, 95% CI = 15.8–44.2%, RR = 24.6). Interestingly, HPV–EBV co-infection was more common in cases with episomal forms of high-risk (HR) HPV whereas HPV alone was more common in cases with integrated HR-HPV. In addition, EBER staining demonstrated that EBV was mainly present in infiltrating lymphocytes. Conclusion Infiltrating EBV-infected lymphocytes may play a role in cancer progression of cervical lesion containing episomal HR-HPV. [ABSTRACT FROM AUTHOR]

Published
2015
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17. HPV16 E2 protein promotes innate immunity by modulating immunosuppressive status.

Author

Sunthamala, Nuchsupha, Pientong, Chamsai, Ohno, Tatsukuni, Zhang, Chenyang, Bhingare, Arundhati, Kondo, Yuta, Azuma, Miyuki, and Ekalaksananan, Tipaya

Subjects
*PAPILLOMAVIRUSES, *VIRAL proteins, *NATURAL immunity, *IMMUNOSUPPRESSION, *KILLER cells, *TUMOR immunology
Abstract

Highlights: [•] HPV16 E2 augments tumor-eradicating innate immune responses mediated by NK cells. [•] HPV16 E2 inhibits myeloid-derived suppressor cells (MDSC) and their-related immunoregulatory mediators. [•] HPV16 E2 may reduce immunoregulatory status in the local microenvironment. [Copyright &y& Elsevier]

Published
2014
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