International Journal of Sports Marketing and Sponsorship
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SCImago
Q2
WOS
Q2
Impact factor
3
SJR
0.596
CiteScore
4.7
Categories
Business and International Management
Finance
Marketing
Sports Science
Areas
Business, Management and Accounting
Economics, Econometrics and Finance
Years of issue
2007-2025
journal names
International Journal of Sports Marketing and Sponsorship
INT J SPORT MARK SPO
Top-3 citing journals

International Journal of Sports Marketing and Sponsorship
(1211 citations)

Sport, Business and Management: An International Journal
(290 citations)

European Sport Management Quarterly
(267 citations)
Top-3 organizations

University of Florida
(17 publications)

University of Lisbon
(9 publications)

Florida State University
(8 publications)

Indiana University Bloomington
(6 publications)

Waseda University
(5 publications)

Georgia State University
(4 publications)
Top-3 countries
Most cited in 5 years
Found
Publications found: 2335

A non-synonymous variant rs12614 of complement factor B associated with risk of chronic hepatitis B in a Korean population
Seo J.Y., Shin J., Youn B.J., Namgoong S., Cheong H.S., Kim L.H., Kim J.O., Shin H.D., Kim Y.J.
Hepatitis B is known to cause several forms of liver diseases including chronic hepatitis B (CHB), and hepatocellular carcinoma. Previous genome-wide association study of CHB risk has demonstrated that rs12614 of complement factor B (CFB) was significantly associated with CHB risk. In this study, fine-mapping study of previously reported GWAS single nucleotide polymorphism (SNP; CFB rs12614) was performed to validate genetic effect of rs12614 on CHB susceptibility and identify possible additional causal variants around rs12614 in a Korean population. This association study was conducted in order to identify genetic effects of CFB single nucleotide polymorphisms (SNPs) and to identify additional independent CHB susceptible causal markers within a Korean population. A total of 10 CFB genetic polymorphisms were selected and genotyped in 1716 study subjects comprised of 955 CHB patients and 761 population controls. A non-synonymous variant, rs12614 (Arg32Trp) in exon2 of CFB, had significant associations with risk of CHB (odds ratio = 0.43, P = 5.91 × 10− 10). Additional linkage disequilibrium and conditional analysis confirmed that rs12614 had independent genetic effect on CHB susceptibility with previously identified CHB markers. The genetic risk scores (GRSs) were calculated and the CHB patients had higher GRSs than the population controls. Moreover, OR was found to increase significantly with cumulative GRS. rs12614 showed significant genetic effect on CHB risk within the Korean population. As such rs12614 may be used as a possible causal genetic variant for CHB susceptibility.

Application of next generation sequencing in genetic counseling a case of a couple at risk of cystinosis
Ouhenach M., Zrhidri A., Jaouad I.C., Smaili W., Sefiani A.
In Morocco, consanguinity rate is very high; which lead to an increase in the birth prevalence of infants with autosomal recessive disorders. Previously, it was difficult to diagnose rare autosomal recessive diseases. Next Generation Sequencing (NGS) techniques have considerably improved clinical diagnostics. A genetic diagnosis showing biallelic causative mutations is the requirement for targeted carrier testing in parents, prenatal and preimplantation genetic diagnosis in further pregnancies, and also for targeted premarital testing in future couples at risk of producing affected children by a known autosomal recessive disease. In this report, we present our strategy to advise a future couple of first cousins, whose descendants would risk cystinosis; an autosomal recessive lysosomal disease caused by mutations in the CTNS gene. Indeed, our future husband’s sister is clinically and biochemically diagnosed with cystinosis in early childhood. First, we opted to identify the patient’s CTNS gene abnormality by using (NGS), then we searched for heterozygosity in the couple’s DNA, which allows us to predict the exact risk of this familial disease in the future couple’s offspring. We have shown that the future husband, brother of the patient is heterozygous for the familial mutation. On the other hand, his future wife did not inherit the familial mutation. Therefore, genetic counseling was reassuring for the risk of familial cystinosis in this couple’s offspring. We report in this study, one of the major applications of (NGS), an effective tool to improve clinical diagnosis and to provide the possibility of targeted premarital carrier testing in couples at risk.

DGAT1 mutations leading to delayed chronic diarrhoea: a case report
Xu L., Gu W., Luo Y., Lou J., Chen J.
Early-onset chronic diarrhoea often indicates a congenital disorder. Mutation in diacylglycerol o-acyltransferase 1 (DGAT1) has recently been linked to early-onset chronic diarrhoea. To date, only a few cases of DGAT1 deficiency have been reported. Diarrhoea in those cases was severe and developed in the neonatal period or within 2 months after birth. Here, we report a female patient with DGAT1 mutations with delayed-onset chronic diarrhoea. The patient had vomiting, hypoalbuminemia, hypertriglyceridemia, and failure to thrive at early infancy. Her intractable chronic diarrhoea occurred until she was 8 months of age. A compound heterozygous DGAT1 mutation was found in the patient, which was first found in the Chinese population. Her symptoms and nutrition status improved after nutritional therapy, including a fat restriction diet. This case expanded our knowledge of the clinical features of patients with DGAT1 mutations. Intractable diarrhoea with delayed onset could also be a congenital disorder.

Case report: progressive familial intrahepatic cholestasis type 3 with compound heterozygous ABCB4 variants diagnosed 15 years after liver transplantation
Goubran M., Aderibigbe A., Jacquemin E., Guettier C., Girgis S., Bain V., Mason A.L.
Progressive familial intrahepatic cholestasis (PFIC) type 3 is an autosomal recessive disorder arising from mutations in the ATP-binding cassette subfamily B member 4 (ABCB4) gene. This gene encodes multidrug resistance protein-3 (MDR3) that acts as a hepatocanalicular floppase that transports phosphatidylcholine from the inner to the outer canalicular membrane. In the absence of phosphatidylcholine, the detergent activity of bile salts is amplified and this leads to cholangiopathy, bile duct loss and biliary cirrhosis. Patients usually present in infancy or childhood and often progress to end-stage liver disease before adulthood. We report a 32-year-old female who required cadaveric liver transplantation at the age of 17 for cryptogenic cirrhosis. When the patient developed chronic ductopenia in the allograft 15 years later, we hypothesized that the patient’s original disease was due to a deficiency of a biliary transport protein and the ductopenia could be explained by an autoimmune response to neoantigen that was not previously encountered by the immune system. We therefore performed genetic analyses and immunohistochemistry of the native liver, which led to a diagnosis of PFIC3. However, there was no evidence of humoral immune response to the MDR3 and therefore, we assumed that the ductopenia observed in the allograft was likely due to chronic rejection rather than autoimmune disease in the allograft. Teenage patients referred for liver transplantation with cryptogenic liver disease should undergo work up for PFIC3. An accurate diagnosis of PFIC 3 is key for optimal management, therapeutic intervention, and avoidance of complications before the onset of end-stage liver disease.

First case report of cerebral folate deficiency caused by a novel mutation of FOLR1 gene in a Chinese patient
Zhang C., Deng X., Wen Y., He F., Yin F., Peng J.
Cerebral folate deficiency (CFD) is a neurological disease, hallmarked by remarkable low concentrations of 5-methyltetrahydrofolic acid (5-MTHF) in cerebrospinal fluid (CSF). The primary causes of CFD include the presence of folate receptor (FR) autoantibodies, defects of FR encoding gene FOLR1, mitochondrial diseases and congenital abnormalities in folate metabolism. Here we first present a Chinese male CFD patient whose seizure onset at 2 years old with convulsive status epilepticus. Magnetic Resonance Imaging (MRI) revealed the development of encephalomalacia, laminar necrosis in multiple lobes of the brain and cerebellar atrophy. Whole Exome Sequencing (WES) uncovered a homozygous missense variant of c.524G > T (p.C175F) in FOLR1 gene. Further laboratory tests demonstrated the extremely low level of 5-MTHF in the CSF from this patient, which was attributed to cerebral folate transport deficiency. Following the intravenous and oral treatment of calcium folinate, the concentrations of 5-MTHF in CSF were recovered to the normal range and seizure symptoms were relieved as well. One novel variation of FOLR1 was firstly identified from a Chinese male patient with tonic-clonic seizures, developmental delay, and ataxia. The WES and laboratory results elucidated the etiology of the symptoms. Clinical outcomes were improved by early diagnosis and proper treatment.

Two novel mutations in the DNAH11 gene in primary ciliary dyskinesia (CILD7) with considerable variety in the clinical and beating cilia phenotype
Schultz R., Elenius V., Lukkarinen H., Saarela T.
Diagnosis of primary ciliary dyskinesia (PCD) still remains a challenge, especially with mutations in the Dynein Arm Heavy Chain 11 (DNAH11) gene. Classical diagnostic measures like Transmission Electron Microscopy (TEM) are not applicable for mutations in the DNAH11 gene since ultrastructural defects of the ciliary apparatus are absent. Novel mutations encoding for PCD appear all the time with considerable variation in the clinical picture, making it necessary to update data bases and guidelines for PCD diagnostics. In this study we examined two unrelated, Finnish families with symptoms of PCD applying the clinical scoring system: Primary ciliary dyskinesia Rule (PICADAR), high speed video microscopy analysis (HSVMA) for ciliary movement, a commercially available gene panel analysis and nasal Nitric Oxide (nNO) measurements if applicable. Two, likely pathogenic variants in the DNAH11 gene (c.2341G > A, p. (Glu781Lys) ja c.7645 + 5G > A) were detected. In the first family, compound heterozygous mutations led to disease manifestation in two of 4 children, which showed a similar phenotype of cilia beating pattern but marked differences in disease severity. In the second family, all three children were homozygotes for the c.2341G > A p.(Glu781Lys) mutation and showed a similar degree of disease severity. However, the phenotype of cilia beating pattern was different ranging from stiff, static cilia to a hyperkinetic movement in one of these children. In this study we describe two Finnish families with PCD, revealing two novel mutations in the DNAH11 gene which show considerable variety in the clinical and beating cilia phenotype. The results of this study show the clinician that PCD can be much milder than generally expected and diagnosis demands a combination of measures which are only successful in experienced hands. Chronic and repeatedly treated wet cough should raise suspicion of PCD, referring the patient for further diagnostics to a specialised PCD centre.

First submicroscopic inversion of the OPA1 gene identified in dominant optic atrophy – a case report
Weisschuh N., Mazzola P., Heinrich T., Haack T., Wissinger B., Tonagel F., Kelbsch C.
Dominant optic atrophy (DOA) is an inherited optic neuropathy that mainly affects visual acuity, central visual fields and color vision due to a progressive loss of retinal ganglion cells and their axons that form the optic nerve. Approximately 45–90% of affected individuals with DOA harbor pathogenic variants in the OPA1 gene. The mutation spectrum of OPA1 comprises nonsense, canonical and non-canonical splice site, frameshift and missense as well as copy number variants, but intragenic inversions have not been reported so far. We report a 33-year-old male with characteristic clinical features of DOA. Whole-genome sequencing identified a structural variant of 2.4 kb comprising an inversion of 937 bp at the OPA1 locus. Fine mapping of the breakpoints to single nucleotide level revealed that the structural variation was an inversion flanked by two deletions. As this rearrangement inverts the entire first exon of OPA1, it was classified as likely pathogenic. We report the first DOA case harboring an inversion in the OPA1 gene. Our study demonstrates that copy-neutral genomic rearrangements have to be considered as a possible cause of disease in DOA cases.

Genome-wide association study of prevalent and persistent cervical high-risk human papillomavirus (HPV) infection
Adebamowo S.N., Adeyemo A.A., Rotimi C.N., Olaniyan O., Offiong R., Adebamowo C.A.
Genetic factors may influence the susceptibility to high-risk (hr) human papillomavirus (HPV) infection and persistence. We conducted the first genome-wide association study (GWAS) to identify variants associated with cervical hrHPV infection and persistence. Participants were 517 Nigerian women evaluated at baseline and 6 months follow-up visits for HPV. HPV was characterized using SPF10/LiPA25. hrHPV infection was positive if at least one carcinogenic HPV genotype was detected in a sample provided at the baseline visit and persistent if at least one carcinogenic HPV genotype was detected in each of the samples provided at the baseline and follow-up visits. Genotyping was done using the Illumina Multi-Ethnic Genotyping Array (MEGA) and imputation was done using the African Genome Resources Haplotype Reference Panel. Association analysis was done for hrHPV infection (125 cases/392 controls) and for persistent hrHPV infection (51 cases/355 controls) under additive genetic models adjusted for age, HIV status and the first principal component (PC) of the genotypes. The mean (±SD) age of the study participants was 38 (±8) years, 48% were HIV negative, 24% were hrHPV positive and 10% had persistent hrHPV infections. No single variant reached genome-wide significance (p < 5 X 10− 8). The top three variants associated with hrHPV infections were intronic variants clustered in KLF12 (all OR: 7.06, p = 1.43 × 10− 6). The top variants associated with cervical hrHPV persistence were in DAP (OR: 6.86, p = 7.15 × 10− 8), NR5A2 (OR: 3.65, p = 2.03 × 10− 7) and MIR365–2 (OR: 7.71, p = 2.63 × 10− 7) gene regions. This exploratory GWAS yielded suggestive candidate risk loci for cervical hrHPV infection and persistence. The identified loci have biological annotation and functional data supporting their role in hrHPV infection and persistence. Given our limited sample size, larger discovery and replication studies are warranted to further characterize the reported associations.

Next generation sequencing of RB1gene for the molecular diagnosis of ethnic minority with retinoblastoma in Yunnan
Zhang Z., Xiao Y., Shen R., Jiang H., Tan L., Li R., Yang X., Gu H., He W., Ma J.
Retinoblastoma is a rare intraocular malignancy and typically initiated by inactivating biallelic mutations of RB1 gene. Each year, ~ 8000 children worldwide are diagnosed for retinoblastoma. In high-income countries, patient survival is over 95% while low-income countries is ~ 30%.If disease is diagnosed early and treated in centers specializing in retinoblastoma, the survival might exceed 95% and many eyes could be safely treated and support a lifetime of good vision. In China, approximate 1100 newly diagnosed cases are expected annually and 28 hospitals covering 25 provinces established centers classified by expertise and resources for better treatment options and follow-up. Comparing with other province of eastern China, Yunnan province is remote geographically. This might result that healthcare staff have low awareness of the role of genetic testing in management and screening in families. The patients with retinoblastoma were selected in Yunnan. DNA from blood was used for targeted gene sequencing. Then, an in-house bioinformatics pipeline was done to detect both single nucleotide variants and small insertions/deletions. The pathogenic mutations were identified and further confirmed by conventional methods and cosegregation in families. Using our approach, targeted next generation sequencing was used to detect the mutation of these 12 probands. Bioinformatic predictions showed that nine mutations were found in our study and four were novel pathogenic variants in these nine mutations. It’s the first report to describe RB1 mutations in Yunnan children with retinoblastoma. This study would improve role of genetic testing for management and family screening.

Mice lacking global Stap1 expression do not manifest hypercholesterolemia
Kanuri B., Fong V., Haller A., Hui D.Y., Patel S.B.
Autosomal dominant familial hypercholesterolemia (ADH; MIM#143890) is one of the most common monogenic disorders characterized by elevated circulatory LDL cholesterol. Initial studies in humans with ADH identified a potential relationship with variants of the gene encoding signal transducing adaptor family member protein 1 (STAP1; MIM#604298). However, subsequent studies have been contradictory. In this study, mice lacking global Stap1 expression (Stap1−/−) were characterized under standard chow and a 42% kcal western diet (WD). Mice were studied for changes in different metabolic parameters before and after a 16-week WD regime. Growth curves, body fats, circulatory lipids, parameters of glucose homeostasis, and liver architecture were studied for comparisons. Surprisingly, Stap1−/− mice fed the 16-week WD demonstrated no marked differences in any of the metabolic parameters compared to Stap1+/+ mice. Furthermore, hepatic architecture and cholesterol content in FPLC-isolated lipoprotein fractions also remained comparable to wild-type mice. These results strongly suggest that STAP1 does not alter lipid levels, that a western diet did not exacerbate a lipid disorder in Stap1 deficient mice and support the contention that it is not causative for hyperlipidemia in ADH patients. These results support other published studies also questioning the role of this locus in human hypercholesterolemia.

Interleukin-4 gene polymorphism (C33T) and the risk of the asthma: a meta-analysis based on 24 publications
Imani D., Eslami M.M., Anani-Sarab G., Aliyu M., Razi B., Rezaei R.
Previous studies evaluated the association of IL-4 C33T polymorphism and risk of bronchial asthma but failed to establish a consistent conclusive association. In the present meta-analysis, we intend to define a more reliable estimate of the association in the presence of filling published literature. An exhaustive search in Web of Science, Scopus, and PubMed databases was performed to identify all relevant publications before September 2020, and 24 publications (28 studies) with 6587 cases and 8408 controls were included in final analysis. The association between polymorphism and risk of asthma were measured by Odd ratios (ORs) and 95% confidence intervals (CIs). Moreover, Cochran’s Q and the I2 statistics were used to evaluate the degree of heterogeneity between studies. In the overall study populations, a significant positive association was detected under all genotype models and announced the IL-4 C33T polymorphism as a potential risk factor in the pathogenesis of asthma. In the subgroup analysis by age, a significant association between IL-4 C33T polymorphism and risk of asthma in different age groups was identified in allelic model, which highlighted the predisposing role of the T allele for the asthma risk in all three age groups. Furthermore, the results of subgroup analysis by continent were heterogenous. Accordingly, IL-4 C33T polymorphism was a risk factor in Europeans (all models except heterozygote comparison), Americans (all models except recessive and homozygote comparison) and Asians (just recessive and allelic model). Finally, the ethnicity-specific analysis disclosed a significant association between IL-4 C33T polymorphism and asthma risk in Caucasians (all genotype models except heterozygote comparison), while this association was not significant in African-Americans. This study suggests that IL-4 C33T polymorphism potentially acts as a risk factor for asthma in different ethnicities and age groups.

Incidence of Huntington disease in a northeastern Spanish region: a 13-year retrospective study at tertiary care centre
Sienes Bailo P., Lahoz R., Sánchez Marín J.P., Izquierdo Álvarez S.
Despite the progress in the knowledge of Huntington disease (HD) in recent years, the epidemiology continues uncertain, so the study of incidence becomes relevant. This is important since various factors (type of population, diagnostic criteria, disease-modifying factors, etc.) make these data highly variable. Therefore, the genetic diagnosis of these patients is important, since it unequivocally allows the detection of new cases. Descriptive retrospective study with 179 individuals. Incidence of HD was calculated from the ratio of number of symptomatic cases newly diagnosed per 100,000 inhabitants per year during the period 2007–2019 in Aragon (Spain). 50 (27.9%) incident cases of HD (CAG repeat length ≥ 36) were identified from a total of 179 persons studied. The remaining 129/179 (72.1%) were HD negative (CAG repeat length < 36). 29 (58.0%) females and 21 (42.0%) males were confirmed as HD cases. The overall incidence was 0.648 per 100,000 patient-years. 11/50 positive HD cases (22.0%) were identified by performing a predictive test, without clinical symptoms. The minimum number of CAG repeats found was 9 and the most common CAG length among HD negative individuals was 16. Our incidence lied within the range reported for other Caucasian populations. Implementation of new techniques has allowed to determine the exact number of CAG repeats, which is especially important in patients with triplet expansions in an HD intermediate and/or incomplete penetrance allele, both in diagnostic, predictive and prenatal tests.

Mediation by differential DNA methylation of known associations between single nucleotide polymorphisms and bladder cancer risk
Jordahl K.M., Phipps A.I., Randolph T.W., Tinker L.F., Nassir R., Hou L., Anderson G.L., Kelsey K.T., White E., Bhatti P.
Though bladder cancer has been the subject of many well-powered genome-wide association studies, the mechanisms involving bladder-cancer-associated single nucleotide polymorphisms (SNPs) remain largely unknown. This study focuses on rs798766, rs401681, rs2294008, and rs8102137, which have been associated with bladder cancer and are also cis-acting methylation quantitative loci (mQTL). Among 412 bladder cancer cases and 424 controls from the Women’s Health Initiative (WHI), we assessed whether the effects of these SNPs on bladder cancer are mediated through proximal DNA methylation changes in pre-diagnostic blood at mQTL-associated CpG sites, which we refer to as natural indirect effects (NIEs). We used a multiple-mediator mediation model for each of the four mQTL adjusted for matching variables and potential confounders, including race/ethnicity, smoking status, and pack-years of smoking. While not statistically significant, our results suggest that substantial proportions of the modest effects of rs401681 (ORNIE = 1.05, 95% confidence interval (CI) = 0.89 to 1.25; NIE percent = 98.5%) and rs2294008 (ORNIE = 1.10, 95% CI = 0.90 to 1.33; NIE percent = 77.6%) on bladder cancer risk are mediated through differential DNA methylation at nearby mQTL-associated CpG sites. The suggestive results indicate that rs2294008 may affect bladder cancer risk through a set of genes in the lymphocyte antigen 6 family, which involves genes that bind to and modulate nicotinic acetylcholine receptors. There was no suggestive evidence supporting mediation for rs8102137 and rs798766. Though larger studies are necessary, the methylation changes associated with rs401681 and rs2294008 at mQTL-associated CpG sites may be relevant for bladder carcinogenesis, and this study demonstrates how multi-omic data can be integrated to help understand the downstream effects of genetics variants.

Overwhelming sepsis in a neonate affected by Zellweger syndrome due to a compound heterozygosis in PEX 6 gene: a case report
Lucaccioni L., Righi B., Cingolani G.M., Lugli L., Della Casa E., Torcetta F., Iughetti L., Berardi A.
Peroxisome biogenesis disorders (PBDs) are a group of metabolic diseases caused by dysfunction of peroxisomes. Different forms of PBDs are described; the most severe one is the Zellweger syndrome (ZS). We report on an unusual presentation of Zellweger syndrome manifesting in a newborn with severe and fulminant sepsis, causing death during the neonatal period. A term male Caucasian neonate presented at birth with hypotonia and poor feeding associated with dysmorphic craniofacial features and skeletal abnormalities. Blood tests showed progressive leukopenia; ultrasounds revealed cerebral and renal abnormalities. He died on the fourth day of life because of an irreversible Gram-negative sepsis. Post-mortem tests on blood and urine samples showed biochemical alterations suggestive of ZS confirmed by genetic test. ZS is an early and severe forms of PBDs. Peroxisomes are known to be involved in lipid metabolism, but recent studies suggest their fundamental role in modulating immune response and inflammation. In case of clinical suspicion of ZS it is important to focus the attention on the prevention and management of infections that can rapidly progress to death.
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International Journal of Sports Marketing and Sponsorship
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IGI Global
237 citations, 3.21%
|
|
Wiley
171 citations, 2.31%
|
|
Frontiers Media S.A.
157 citations, 2.12%
|
|
Walter de Gruyter
82 citations, 1.11%
|
|
Cognizant, LLC
62 citations, 0.84%
|
|
Institute of Electrical and Electronics Engineers (IEEE)
51 citations, 0.69%
|
|
Social Science Electronic Publishing
42 citations, 0.57%
|
|
Japanese Association for Sport Management
33 citations, 0.45%
|
|
World Scientific
23 citations, 0.31%
|
|
Japan Society of Sports Industry
20 citations, 0.27%
|
|
Association for Computing Machinery (ACM)
19 citations, 0.26%
|
|
Public Library of Science (PLoS)
18 citations, 0.24%
|
|
Hindawi Limited
18 citations, 0.24%
|
|
Cambridge University Press
16 citations, 0.22%
|
|
JMIR Publications
16 citations, 0.22%
|
|
LLC CPC Business Perspectives
12 citations, 0.16%
|
|
SciELO
11 citations, 0.15%
|
|
CAIRN
10 citations, 0.14%
|
|
Japan Marketing Academy
10 citations, 0.14%
|
|
Vilnius Gediminas Technical University
9 citations, 0.12%
|
|
IOP Publishing
9 citations, 0.12%
|
|
Bentham Science Publishers Ltd.
8 citations, 0.11%
|
|
Centre for Evaluation in Education and Science (CEON/CEES)
8 citations, 0.11%
|
|
Universitas Pendidikan Indonesia
7 citations, 0.09%
|
|
Asian Exercise and Sport Science Association
7 citations, 0.09%
|
|
Fundacao Getulio Vargas, Escola de Administracao de Empresas de Sao Paulo
7 citations, 0.09%
|
|
The Advertising Research Foundation
7 citations, 0.09%
|
|
Academic Journals
7 citations, 0.09%
|
|
AOSIS
7 citations, 0.09%
|
|
South Florida Publishing LLC
7 citations, 0.09%
|
|
Japan Society of Physical Education, Health and Sport Sciences
7 citations, 0.09%
|
|
Oxford University Press
6 citations, 0.08%
|
|
Gazi University
6 citations, 0.08%
|
|
Masaryk University Press
6 citations, 0.08%
|
|
Sociedade Brasileira de Psicologia
6 citations, 0.08%
|
|
Virtus Interpress
6 citations, 0.08%
|
|
OpenEdition
6 citations, 0.08%
|
|
Scientific Research Publishing
6 citations, 0.08%
|
|
Center for Strategic Studies in Business and Finance SSBFNET
6 citations, 0.08%
|
|
American Marketing Association
5 citations, 0.07%
|
|
University of Illinois Press
5 citations, 0.07%
|
|
National Recreation and Park Association
5 citations, 0.07%
|
|
Akademiai Kiado
5 citations, 0.07%
|
|
IntechOpen
5 citations, 0.07%
|
|
Pamukkale University
5 citations, 0.07%
|
|
EDP Sciences
4 citations, 0.05%
|
|
The Japan Section of the Regional Science Association International
4 citations, 0.05%
|
|
Goteborg University
4 citations, 0.05%
|
|
AIP Publishing
3 citations, 0.04%
|
|
Alexandru Ioan Cuza - University of Iasi
3 citations, 0.04%
|
|
Mackenzie Presbyterian University
3 citations, 0.04%
|
|
Sumy State University
3 citations, 0.04%
|
|
Colegio Brasileiro de Ciencias do Esporte (CBCE)
3 citations, 0.04%
|
|
Brazilian Administration Review
3 citations, 0.04%
|
|
John Benjamins Publishing Company
2 citations, 0.03%
|
|
Institute for Operations Research and the Management Sciences (INFORMS)
2 citations, 0.03%
|
|
Academy of Management
2 citations, 0.03%
|
|
Editura Economica
2 citations, 0.03%
|
|
Gyandhara International Academic Publications
2 citations, 0.03%
|
|
Oxford Brookes University
2 citations, 0.03%
|
|
N T C Publications Ltd.
2 citations, 0.03%
|
|
Vilnius University Press
2 citations, 0.03%
|
|
Scandinavian University Press / Universitetsforlaget AS
2 citations, 0.03%
|
|
Intellect
2 citations, 0.03%
|
|
Hans Publishers
2 citations, 0.03%
|
|
IOS Press
1 citation, 0.01%
|
|
Mary Ann Liebert
1 citation, 0.01%
|
|
1 citation, 0.01%
|
|
Hacettepe University
1 citation, 0.01%
|
|
1 citation, 0.01%
|
|
Open Science Center, University of Jyvaskyla
1 citation, 0.01%
|
|
University of Warsaw
1 citation, 0.01%
|
|
Lavoisier
1 citation, 0.01%
|
|
Index Copernicus
1 citation, 0.01%
|
|
Pensoft Publishers
1 citation, 0.01%
|
|
Edizioni Minerva Medica
1 citation, 0.01%
|
|
Tsinghua University Press
1 citation, 0.01%
|
|
North American Society for Sport History
1 citation, 0.01%
|
|
Academy of Physical Education
1 citation, 0.01%
|
|
1 citation, 0.01%
|
|
NP Voprosy Ekonomiki
1 citation, 0.01%
|
|
Society for Personality Research
1 citation, 0.01%
|
|
International Association of Computer Science in Sport
1 citation, 0.01%
|
|
Institute of Asian Studies at the GIGA German Institute of Global and Area Studies
1 citation, 0.01%
|
|
IAE School of Management Montpellier University
1 citation, 0.01%
|
|
Cold Spring Harbor Laboratory
1 citation, 0.01%
|
|
BMJ
1 citation, 0.01%
|
|
American Psychological Association (APA)
1 citation, 0.01%
|
|
EJournal Publishing
1 citation, 0.01%
|
|
ASTM International
1 citation, 0.01%
|
|
Knowledge E DMCC
1 citation, 0.01%
|
|
Publishing House Finance and Credit
1 citation, 0.01%
|
|
A and V Publications
1 citation, 0.01%
|
|
Show all (70 more) | |
500
1000
1500
2000
2500
|
Publishing organizations
2
4
6
8
10
12
14
16
18
|
|
University of Florida
17 publications, 2.11%
|
|
University of Lisbon
9 publications, 1.12%
|
|
Florida State University
8 publications, 1%
|
|
Indiana University Bloomington
8 publications, 1%
|
|
Texas A&M University
8 publications, 1%
|
|
Coventry University
8 publications, 1%
|
|
Seattle University
7 publications, 0.87%
|
|
Georgia State University
7 publications, 0.87%
|
|
Shanghai University of Sport
6 publications, 0.75%
|
|
Laurentian University
6 publications, 0.75%
|
|
De Montfort University
6 publications, 0.75%
|
|
University of Louisville
6 publications, 0.75%
|
|
Université Paris-Saclay
6 publications, 0.75%
|
|
Massey University
5 publications, 0.62%
|
|
Deakin University
5 publications, 0.62%
|
|
Griffith University
5 publications, 0.62%
|
|
University of Leeds
5 publications, 0.62%
|
|
Waseda University
5 publications, 0.62%
|
|
Sheffield Hallam University
5 publications, 0.62%
|
|
Université Laval
5 publications, 0.62%
|
|
University of Memphis
5 publications, 0.62%
|
|
La Trobe University
4 publications, 0.5%
|
|
Korea University
4 publications, 0.5%
|
|
Sungkyunkwan University
4 publications, 0.5%
|
|
Chung-Ang University
4 publications, 0.5%
|
|
University of Texas at Austin
4 publications, 0.5%
|
|
University of Michigan
4 publications, 0.5%
|
|
University of British Columbia
4 publications, 0.5%
|
|
Temple University
4 publications, 0.5%
|
|
University of Miami
4 publications, 0.5%
|
|
University of North Carolina at Chapel Hill
4 publications, 0.5%
|
|
Radboud University Nijmegen
3 publications, 0.37%
|
|
University of Bayreuth
3 publications, 0.37%
|
|
Stockholm University
3 publications, 0.37%
|
|
University of New South Wales
3 publications, 0.37%
|
|
Loughborough University
3 publications, 0.37%
|
|
University of Otago
3 publications, 0.37%
|
|
University of Queensland
3 publications, 0.37%
|
|
University of Adelaide
3 publications, 0.37%
|
|
Seoul National University
3 publications, 0.37%
|
|
Yonsei University
3 publications, 0.37%
|
|
Kyung Hee University
3 publications, 0.37%
|
|
National and Kapodistrian University of Athens
3 publications, 0.37%
|
|
German Sport University Cologne
3 publications, 0.37%
|
|
University of Minnesota
3 publications, 0.37%
|
|
Virginia Commonwealth University
3 publications, 0.37%
|
|
University of Maryland, College Park
3 publications, 0.37%
|
|
University of Alberta
3 publications, 0.37%
|
|
University of Navarra
3 publications, 0.37%
|
|
Northern Kentucky University
3 publications, 0.37%
|
|
University of North Texas
3 publications, 0.37%
|
|
University of Alabama
3 publications, 0.37%
|
|
University of Bath
3 publications, 0.37%
|
|
Hamad Bin Khalifa University
2 publications, 0.25%
|
|
University of Malaya
2 publications, 0.25%
|
|
University of Science, Malaysia
2 publications, 0.25%
|
|
Autonomous University of Lisbon
2 publications, 0.25%
|
|
Nanyang Technological University
2 publications, 0.25%
|
|
National Taiwan Normal University
2 publications, 0.25%
|
|
Tamkang University
2 publications, 0.25%
|
|
National Chung Cheng University
2 publications, 0.25%
|
|
National University of Kaohsiung
2 publications, 0.25%
|
|
Universidade Federal do Rio de Janeiro
2 publications, 0.25%
|
|
Iowa State University
2 publications, 0.25%
|
|
Auckland University of Technology
2 publications, 0.25%
|
|
Monash University
2 publications, 0.25%
|
|
Royal Melbourne Institute of Technology
2 publications, 0.25%
|
|
Swinburne University of Technology
2 publications, 0.25%
|
|
Victoria University (Australia)
2 publications, 0.25%
|
|
Australian Defence Force Academy
2 publications, 0.25%
|
|
Pusan National University
2 publications, 0.25%
|
|
Arizona State University
2 publications, 0.25%
|
|
Hong Kong Metropolitan University
2 publications, 0.25%
|
|
New York University
2 publications, 0.25%
|
|
Vrije Universiteit Brussel
2 publications, 0.25%
|
|
Southern Illinois University Carbondale
2 publications, 0.25%
|
|
University of Illinois Urbana-Champaign
2 publications, 0.25%
|
|
Queen's University at Kingston
2 publications, 0.25%
|
|
Goethe University Frankfurt
2 publications, 0.25%
|
|
Utrecht University
2 publications, 0.25%
|
|
Hosei University
2 publications, 0.25%
|
|
Kutztown University of Pennsylvania
2 publications, 0.25%
|
|
Brock University
2 publications, 0.25%
|
|
University of Ottawa
2 publications, 0.25%
|
|
Miami University
2 publications, 0.25%
|
|
Texas Tech University
2 publications, 0.25%
|
|
Troy University
2 publications, 0.25%
|
|
Old Dominion University
2 publications, 0.25%
|
|
University of Tennessee
2 publications, 0.25%
|
|
Sacred Heart University
2 publications, 0.25%
|
|
University of Stirling
2 publications, 0.25%
|
|
University of Salford
2 publications, 0.25%
|
|
King Abdulaziz University
1 publication, 0.12%
|
|
Boğaziçi University
1 publication, 0.12%
|
|
Istanbul University
1 publication, 0.12%
|
|
Ajman University of Science and Technology
1 publication, 0.12%
|
|
Karamanoğlu Mehmetbey University
1 publication, 0.12%
|
|
Islamic Azad University, Tehran
1 publication, 0.12%
|
|
Islamic Azad University, Karaj
1 publication, 0.12%
|
|
Urmia University
1 publication, 0.12%
|
|
Show all (70 more) | |
2
4
6
8
10
12
14
16
18
|
Publishing organizations in 5 years
1
2
3
4
5
6
|
|
Indiana University Bloomington
6 publications, 2.16%
|
|
Waseda University
5 publications, 1.8%
|
|
Georgia State University
4 publications, 1.44%
|
|
Texas A&M University
4 publications, 1.44%
|
|
University of Lisbon
3 publications, 1.08%
|
|
University of Bayreuth
3 publications, 1.08%
|
|
La Trobe University
3 publications, 1.08%
|
|
Seattle University
3 publications, 1.08%
|
|
University of Michigan
3 publications, 1.08%
|
|
Temple University
3 publications, 1.08%
|
|
University of Florida
3 publications, 1.08%
|
|
University of Bath
3 publications, 1.08%
|
|
Hamad Bin Khalifa University
2 publications, 0.72%
|
|
Autonomous University of Lisbon
2 publications, 0.72%
|
|
Florida State University
2 publications, 0.72%
|
|
Loughborough University
2 publications, 0.72%
|
|
Tamkang University
2 publications, 0.72%
|
|
Universidade Federal do Rio de Janeiro
2 publications, 0.72%
|
|
Sungkyunkwan University
2 publications, 0.72%
|
|
Hong Kong Metropolitan University
2 publications, 0.72%
|
|
German Sport University Cologne
2 publications, 0.72%
|
|
Virginia Commonwealth University
2 publications, 0.72%
|
|
University of Miami
2 publications, 0.72%
|
|
University of North Carolina at Chapel Hill
2 publications, 0.72%
|
|
Miami University
2 publications, 0.72%
|
|
University of North Texas
2 publications, 0.72%
|
|
Old Dominion University
2 publications, 0.72%
|
|
University of Stirling
2 publications, 0.72%
|
|
King Abdulaziz University
1 publication, 0.36%
|
|
Boğaziçi University
1 publication, 0.36%
|
|
Istanbul University
1 publication, 0.36%
|
|
Ajman University of Science and Technology
1 publication, 0.36%
|
|
Karamanoğlu Mehmetbey University
1 publication, 0.36%
|
|
Islamic Azad University, Tehran
1 publication, 0.36%
|
|
Islamic Azad University, Karaj
1 publication, 0.36%
|
|
Urmia University
1 publication, 0.36%
|
|
University of Kurdistan
1 publication, 0.36%
|
|
Koneru Lakshmaiah Education Foundation
1 publication, 0.36%
|
|
Guru Gobind Singh Indraprastha University
1 publication, 0.36%
|
|
Punjabi University
1 publication, 0.36%
|
|
Indian Institute of Information Technology, Allahabad
1 publication, 0.36%
|
|
Qatar University
1 publication, 0.36%
|
|
Katholieke Universiteit Leuven
1 publication, 0.36%
|
|
University of Twente
1 publication, 0.36%
|
|
University of Malaya
1 publication, 0.36%
|
|
The MARA Technological University
1 publication, 0.36%
|
|
Nanjing University of Finance and Economics
1 publication, 0.36%
|
|
University of Bern
1 publication, 0.36%
|
|
Nanyang Technological University
1 publication, 0.36%
|
|
Shanghai University of Sport
1 publication, 0.36%
|
|
Lappeenranta-Lahti University of Technology
1 publication, 0.36%
|
|
Wuhan Sports University
1 publication, 0.36%
|
|
Hohai University
1 publication, 0.36%
|
|
King's College London
1 publication, 0.36%
|
|
University of Antwerp
1 publication, 0.36%
|
|
Manchester Metropolitan University
1 publication, 0.36%
|
|
United International College
1 publication, 0.36%
|
|
Michigan State University
1 publication, 0.36%
|
|
National Taipei University of Technology
1 publication, 0.36%
|
|
National Taiwan Normal University
1 publication, 0.36%
|
|
National Cheng Kung University
1 publication, 0.36%
|
|
National University of Kaohsiung
1 publication, 0.36%
|
|
Tunghai University
1 publication, 0.36%
|
|
Huaqiao University
1 publication, 0.36%
|
|
Iowa State University
1 publication, 0.36%
|
|
Free University of Bozen-Bolzano
1 publication, 0.36%
|
|
University of Bergamo
1 publication, 0.36%
|
|
Auckland University of Technology
1 publication, 0.36%
|
|
University of Queensland
1 publication, 0.36%
|
|
Swinburne University of Technology
1 publication, 0.36%
|
|
North-West University
1 publication, 0.36%
|
|
Washington State University
1 publication, 0.36%
|
|
Yonsei University
1 publication, 0.36%
|
|
Korea University
1 publication, 0.36%
|
|
Arizona State University
1 publication, 0.36%
|
|
North Carolina State University
1 publication, 0.36%
|
|
Chonnam National University
1 publication, 0.36%
|
|
West Virginia University
1 publication, 0.36%
|
|
Sookmyung Womens University
1 publication, 0.36%
|
|
New York University
1 publication, 0.36%
|
|
Pukyong National University
1 publication, 0.36%
|
|
Kongju National University
1 publication, 0.36%
|
|
Illinois State University
1 publication, 0.36%
|
|
Southern Methodist University
1 publication, 0.36%
|
|
Liaoning University
1 publication, 0.36%
|
|
Macau University of Science and Technology
1 publication, 0.36%
|
|
Vrije Universiteit Brussel
1 publication, 0.36%
|
|
National Chiayi University
1 publication, 0.36%
|
|
Western Michigan University
1 publication, 0.36%
|
|
McGill University
1 publication, 0.36%
|
|
Macao Polytechnic University
1 publication, 0.36%
|
|
University of Seville
1 publication, 0.36%
|
|
University of British Columbia
1 publication, 0.36%
|
|
Queen's University at Kingston
1 publication, 0.36%
|
|
Winona State University
1 publication, 0.36%
|
|
University of Innsbruck
1 publication, 0.36%
|
|
Leeds Beckett University
1 publication, 0.36%
|
|
University of Leeds
1 publication, 0.36%
|
|
Vienna University of Economics and Business
1 publication, 0.36%
|
|
University of Porto
1 publication, 0.36%
|
|
Show all (70 more) | |
1
2
3
4
5
6
|
Publishing countries
50
100
150
200
250
|
|
USA
|
USA, 203, 25.25%
USA
203 publications, 25.25%
|
United Kingdom
|
United Kingdom, 54, 6.72%
United Kingdom
54 publications, 6.72%
|
Australia
|
Australia, 36, 4.48%
Australia
36 publications, 4.48%
|
Canada
|
Canada, 32, 3.98%
Canada
32 publications, 3.98%
|
Republic of Korea
|
Republic of Korea, 31, 3.86%
Republic of Korea
31 publications, 3.86%
|
China
|
China, 27, 3.36%
China
27 publications, 3.36%
|
France
|
France, 20, 2.49%
France
20 publications, 2.49%
|
Germany
|
Germany, 17, 2.11%
Germany
17 publications, 2.11%
|
Portugal
|
Portugal, 12, 1.49%
Portugal
12 publications, 1.49%
|
New Zealand
|
New Zealand, 12, 1.49%
New Zealand
12 publications, 1.49%
|
Spain
|
Spain, 10, 1.24%
Spain
10 publications, 1.24%
|
Japan
|
Japan, 9, 1.12%
Japan
9 publications, 1.12%
|
Netherlands
|
Netherlands, 8, 1%
Netherlands
8 publications, 1%
|
Malaysia
|
Malaysia, 6, 0.75%
Malaysia
6 publications, 0.75%
|
Greece
|
Greece, 5, 0.62%
Greece
5 publications, 0.62%
|
India
|
India, 5, 0.62%
India
5 publications, 0.62%
|
Norway
|
Norway, 5, 0.62%
Norway
5 publications, 0.62%
|
Brazil
|
Brazil, 4, 0.5%
Brazil
4 publications, 0.5%
|
Italy
|
Italy, 4, 0.5%
Italy
4 publications, 0.5%
|
Belgium
|
Belgium, 3, 0.37%
Belgium
3 publications, 0.37%
|
Qatar
|
Qatar, 3, 0.37%
Qatar
3 publications, 0.37%
|
Turkey
|
Turkey, 3, 0.37%
Turkey
3 publications, 0.37%
|
Sweden
|
Sweden, 3, 0.37%
Sweden
3 publications, 0.37%
|
Austria
|
Austria, 2, 0.25%
Austria
2 publications, 0.25%
|
Argentina
|
Argentina, 2, 0.25%
Argentina
2 publications, 0.25%
|
Iran
|
Iran, 2, 0.25%
Iran
2 publications, 0.25%
|
Singapore
|
Singapore, 2, 0.25%
Singapore
2 publications, 0.25%
|
South Africa
|
South Africa, 2, 0.25%
South Africa
2 publications, 0.25%
|
Vietnam
|
Vietnam, 1, 0.12%
Vietnam
1 publication, 0.12%
|
Denmark
|
Denmark, 1, 0.12%
Denmark
1 publication, 0.12%
|
Ireland
|
Ireland, 1, 0.12%
Ireland
1 publication, 0.12%
|
UAE
|
UAE, 1, 0.12%
UAE
1 publication, 0.12%
|
Saudi Arabia
|
Saudi Arabia, 1, 0.12%
Saudi Arabia
1 publication, 0.12%
|
Tunisia
|
Tunisia, 1, 0.12%
Tunisia
1 publication, 0.12%
|
Finland
|
Finland, 1, 0.12%
Finland
1 publication, 0.12%
|
Switzerland
|
Switzerland, 1, 0.12%
Switzerland
1 publication, 0.12%
|
Show all (6 more) | |
50
100
150
200
250
|
Publishing countries in 5 years
10
20
30
40
50
60
|
|
USA
|
USA, 55, 19.78%
USA
55 publications, 19.78%
|
China
|
China, 15, 5.4%
China
15 publications, 5.4%
|
United Kingdom
|
United Kingdom, 9, 3.24%
United Kingdom
9 publications, 3.24%
|
Republic of Korea
|
Republic of Korea, 7, 2.52%
Republic of Korea
7 publications, 2.52%
|
Portugal
|
Portugal, 6, 2.16%
Portugal
6 publications, 2.16%
|
Germany
|
Germany, 5, 1.8%
Germany
5 publications, 1.8%
|
Japan
|
Japan, 5, 1.8%
Japan
5 publications, 1.8%
|
Australia
|
Australia, 4, 1.44%
Australia
4 publications, 1.44%
|
India
|
India, 4, 1.44%
India
4 publications, 1.44%
|
Qatar
|
Qatar, 3, 1.08%
Qatar
3 publications, 1.08%
|
France
|
France, 2, 0.72%
France
2 publications, 0.72%
|
Austria
|
Austria, 2, 0.72%
Austria
2 publications, 0.72%
|
Belgium
|
Belgium, 2, 0.72%
Belgium
2 publications, 0.72%
|
Brazil
|
Brazil, 2, 0.72%
Brazil
2 publications, 0.72%
|
Iran
|
Iran, 2, 0.72%
Iran
2 publications, 0.72%
|
Spain
|
Spain, 2, 0.72%
Spain
2 publications, 0.72%
|
Italy
|
Italy, 2, 0.72%
Italy
2 publications, 0.72%
|
Canada
|
Canada, 2, 0.72%
Canada
2 publications, 0.72%
|
Malaysia
|
Malaysia, 2, 0.72%
Malaysia
2 publications, 0.72%
|
Turkey
|
Turkey, 2, 0.72%
Turkey
2 publications, 0.72%
|
Vietnam
|
Vietnam, 1, 0.36%
Vietnam
1 publication, 0.36%
|
Netherlands
|
Netherlands, 1, 0.36%
Netherlands
1 publication, 0.36%
|
New Zealand
|
New Zealand, 1, 0.36%
New Zealand
1 publication, 0.36%
|
UAE
|
UAE, 1, 0.36%
UAE
1 publication, 0.36%
|
Saudi Arabia
|
Saudi Arabia, 1, 0.36%
Saudi Arabia
1 publication, 0.36%
|
Singapore
|
Singapore, 1, 0.36%
Singapore
1 publication, 0.36%
|
Finland
|
Finland, 1, 0.36%
Finland
1 publication, 0.36%
|
Switzerland
|
Switzerland, 1, 0.36%
Switzerland
1 publication, 0.36%
|
South Africa
|
South Africa, 1, 0.36%
South Africa
1 publication, 0.36%
|
10
20
30
40
50
60
|