Next Article in Journal
Understanding Merkel Cell Carcinoma: Pathogenic Signaling, Extracellular Matrix Dynamics, and Novel Treatment Approaches
Next Article in Special Issue
Rectovaginal Extra-Gastrointestinal Stromal Tumors (EGISTs): A Systematic Review of the Literature and a Pooled Survival Analysis
Previous Article in Journal
Tumor Treating Fields and Combination Therapy in Management of Brain Oncology
Previous Article in Special Issue
Does Total Neoadjuvant Therapy Impact Surgical Precision in Total Mesorectal Excision? A Nationwide Survey of the Experiences of Expert Surgeons
 
 
Search for Articles:
Title / Keyword
Author / Affiliation / Email
Journal
Article Type
 
 
Advanced Search
 
Section
Special Issue
Volume
Issue
Number
Page
 
Journals
Cancers
Volume 17
Issue 7
10.3390/cancers17071209
cancers-logo
Submit to this Journal Review for this Journal Propose a Special Issue
Article Menu

Article Menu

share Share announcement Help format_quote Cite question_answer Discuss in SciProfiles
first_page
settings
Order Article Reprints
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Article

Inflammatory Fibroid Polyp (Vanek’s Tumor): A Retrospective Multicentric Analysis of 67 Cases

by
Mario Martín Sánchez
1,†,
Víctor Domínguez-Prieto
1,†,
Siyuan Qian Zhang
1,*,
Hernán Darío Quiceno Arias
2,
María Bernarda Álvarez Álvarez
2,
Montiel Jiménez Fuertes
1,
Cecilia Meliga
1,
Santos Jiménez-Galanes
3,
Héctor Guadalajara Labajo
1,4,
Damián García Olmo
1,4 and
Pedro Villarejo Campos
1,4
1
Department of Surgery, Fundación Jiménez Díaz University Hospital, Avenida de los Reyes Católicos 2, 28040 Madrid, Spain
2
Department of Pathology, Fundación Jiménez Díaz University Hospital, Avenida de los Reyes Católicos 2, 28040 Madrid, Spain
3
Department of Surgery, University Hospital Infanta Elena, 28342 Madrid, Spain
4
Department of Surgery, Universidad Autónoma de Madrid, 28049 Madrid, Spain
*
Author to whom correspondence should be addressed.
These authors contributed equally to this work.
Cancers 2025, 17(7), 1209; https://doi.org/10.3390/cancers17071209
Submission received: 4 March 2025 / Revised: 30 March 2025 / Accepted: 1 April 2025 / Published: 2 April 2025
(This article belongs to the Special Issue Gastrointestinal Cancer Surgery)
Versions Notes

Simple Summary

Inflammatory fibroid polyps, also known as Vanek’s tumors, are rare benign lesions of the gastrointestinal tract that can mimic malignant conditions, posing a diagnostic challenge. This study presents the largest multicentric analysis of these tumors to date, aiming to characterize their clinical presentation, anatomical distribution, and management strategies. We provide valuable insights into the effectiveness of endoscopic and surgical approaches, particularly in relation to tumor location and size. Our findings may contribute to optimizing diagnostic accuracy, guiding treatment decisions, and reducing unnecessary surgical interventions.

Abstract

Objectives: Inflammatory fibroid polyps, also known as Vanek’s tumors, are rare benign lesions of the gastrointestinal tract. Although the exact cause remains unclear, several theories suggest an association with inflammatory processes and genetic factors. This study aims to present the largest cohort of inflammatory fibroid polyp cases to date, analyzing their clinical presentation, diagnostic methods, and treatment approaches. Materials and methods: A retrospective multicentric analysis was conducted on 67 patients diagnosed with inflammatory fibroid polyps between 2013 and 2023 across four hospitals. Clinical data regarding tumor location, size, symptoms, and treatment were collected. Non-parametric statistical tests, including the chi-square test, Cramér’s V coefficient, and the Mann–Whitney U test, were used to identify association between tumor characteristics, location, and treatment outcomes. Results: The cohort included 67 patients (58.2% female, median age 60 years). The stomach was the most common tumor site (47.8%), followed by the colon (32.8%), and small intestine (10.4%). The majority of patients (73.1%) were asymptomatic, while 9% experienced intestinal obstruction, all of which were located in the small intestine. Endoscopic resection was successful in 77.6% of cases, but surgical intervention was more frequently required for tumors in the small intestine. A significant association was found between larger tumor size, emergency presentation, intestinal location, and the need for surgery. Conclusions: Inflammatory fibroid polyps are commonly managed with endoscopic resection, particularly in gastric and colonic locations. However, small intestinal tumors more often need surgical treatment, especially when presenting with complications like intestinal obstruction.

1. Introduction

Inflammatory fibroid polyp (IFP), also known as Vanek’s tumor, was first documented by J. Vanek in 1949. This publication included six patients with diverse clinical presentations in whom he identified a peculiar submucosal gastric lesion described as a “submucosal granuloma with an eosinophilic infiltration” [1]. These tumors are defined as benign, idiopathic, and localized neoplastic lesions in the submucosa of gastrointestinal (GI) tract [2].
Vanek’s tumor represents less than 0.1% of all gastric polyps [3]. Epidemiologically, IFP affects both sexes equally. It has a wide age range, with a peak of incidence in the fifth to seventh decades of life.
In the anatomopathological examination, IFPs are pedunculated or sessile lesions that vary in size, often projecting into the bowel lumen. Microscopically, these lesions are characterized by a spindle and stellate cell proliferation within a fibrous or myxoid stroma, highly vascular, and accompanied with significant inflammatory infiltrate, predominantly eosinophilic [2,4].
Immunohistochemically, Vanek’s tumors consistently express CD34 and vimentin while lacking CD117. This distinctive profile is crucial for distinguishing IFP from GIST and other mesenchymal tumors that may share similar morphological features [5,6]. At the molecular level, significant advances have identified activating mutations in the platelet-derived growth factor receptor alpha (PDGFRA) gene in up to 70% of IFPs [7,8]. However, the presence of PDGFRA mutations in both IFP and a subset of GISTs may complicate the differential diagnosis, particularly in cases where GIST lacks CD117 expression [9].
Although they can be found throughout the GI tract, IFPs are commonly located at the gastric antrum or ileum. They are typically asymptomatic. When present, clinical manifestations can vary according to size and location: abdominal pain is frequently observed with IFPs located in the stomach, while obstruction and intussusception are more characteristic when the tumor is found in the small intestine [10,11,12,13]. Colonic IFP, in contrast, may resemble symptoms of a malignant tumor such as iron deficiency anemia, hematochezia, or change in bowel habits [14,15].
Radiological imaging such as ultrasonography, computer tomography (CT) or magnetic resonance imaging (MRI) are commonly used for diagnosis of IFP’s complications. Regarding treatment, most IFPs are diagnosed and treated by endoscopic resection [16,17,18]. Surgical intervention is reserved for cases where endoscopic resection is not feasible due to tumor size or location. Furthermore, sometimes urgent surgery is needed primarily in case of intussusception or obstruction [19,20,21].
Most available studies on IFP are based on small retrospectives series, limiting the ability to draw definitive conclusions regarding their clinical behavior and management [22,23].
To our knowledge, this study represents the largest cohort of patients with Vanek’s tumor reported to date. By documenting our findings, we aim to provide a comprehensive analysis of IFP by investigating its clinical presentation, diagnostic modalities, and treatment options. This study seeks to enhance the understanding of this rare entity and contribute to establishing more consistent diagnostic and therapeutic strategies.

2. Materials and Methods

A multicenter retrospective analysis was conducted on all patients diagnosed histologically with IFP or Vanek’s tumor from 2013 to 2023 from four hospitals in Madrid (Spain): Hospital Universitario Fundación Jiménez Díaz, Hospital Universitario Rey Juan Carlos, Hospital Universitario General de Villalba, and Hospital Universitario Infanta Elena. The participating centers included one tertiary referral hospital (Hospital Universitario Fundación Jiménez Díaz) and three secondary-level hospitals, collectively serving a population of approximately 850,000 inhabitants within the Madrid region.

2.1. Patient Selection and Data Collection

Patients were identified through a comprehensive review of pathological databases across the participating institutions. Most diagnoses were established incidentally through endoscopic procedures, while others were obtained from surgical specimens. Currently, there are no universally standardized diagnosis criteria for IFP. However, all cases were analyzed by experienced pathologists following histopathological criteria to ensure diagnostic accuracy and consistency across centers.
All participating centers had access to the same diagnostic and therapeutic resources, ensuring a uniform approach to patient management. In the absence of standardized guidelines, treatment decisions were based on clinical judgment and institutional protocols, which were comparable across all hospitals.
Clinical data were retrospectively collected from electronic medical records and institutional databases. Patients were identified based on histopathological reports confirming IFPs. The information gathered included patient demographics (age and sex), tumor characteristics (size, location, histological findings), clinical presentation, diagnosis, treatment approach, and follow-up. Exclusion criteria included cases with incomplete medical records or cases with diagnostic uncertainty after histological examination.

2.2. Statistical Analysis

Initially, the Kolmogorov–Smirnov (KS) test was applied to assess the normality distribution of all variables. In this study, all variables resulted in a KS test p < 0.05, leading to the application of non-parametric tests.
The Kruskal–Wallis test was used to compare the relationship between the categorical and the continuous variables. The chi-square ( χ 2 ) test was employed to compare two qualitative variables. Therefore, Cramér’s V coefficient was applied to evaluate the strength of the association, with values closer to 1 indicating a stronger association. The Mann–Whitney U test was utilized as a non-parametric test to analyze relationships between quantitative and qualitative variables. Additionally, Cohen’s R was used to quantify the effect size in this comparison. Statistical significance was set at p < 0.05.
The statistical analyses were performed using SPSS software, version 25.

3. Results

A total of 67 patients were included, consisting of 39 females (58.2%) and 28 males (41.8%), with a median age of 60 years (range 32–83 years).

3.1. Tumor Location

Regarding tumor location (Table 1), the stomach was the main location, involving 32 patients (47.8%). Vanek’s tumor was diagnosed in 22 patients (32.8%) in the large intestine, while 7 patients (10.4%) had the tumor located in the small intestine. Additionally, the rectum was affected in 5 patients (7.5%), and the esophagus in 1 patient (1.5%).
The most common site in the stomach was the antrum, observed in 25 patients (78.1% of gastric IFPs). The pylorus and corpus were affected in 4 and 3 patients, respectively (12.5% and 9.4% of gastric IFPs). Regarding colonic IFP, 17 patients (77.3% of colonic IFPs) had IFP localized in the left colon, 3 patients (13.6% of colonic IFP) in the right colon and 2 patients (9.1% of colonic IFPs) in the transverse colon.
In relation to tumor location and demographic characteristics (Table 2), among male patients, 12 patients (42.9%) had gastric IFPs, 9 patients (32.1%) had colonic IFPs, 4 patients (14.3%) had rectal IFPs, and 2 patients (7.1%) had small intestine lesions. In contrast, among female patients, 20 patients (51.3%) had gastric IFPs, 13 patients (33.3%) had colonic IFPs, 5 patients (12.8%) had small intestine lesions, and 1 patient (2.6%) had a rectal lesion. The only esophageal IFP was observed in a male patient. There was no statistically significant association between tumor location and sex (p = 0.282).
The mean age of the patients varied across different tumor locations. The highest mean age was observed in patients with tumors located in the stomach (63 years), followed by those with tumors in the colon (59 years). Patients with esophageal tumors had a mean age of 57 years, while those with tumors in the rectum (56 years) and small intestine (55 years) had the lowest mean ages. However, no statistically significant relationship was found between age and tumor location (p = 0.488).

3.2. Clinical Presentation

The majority of diagnoses were incidental, with 49 patients (73.1%) being asymptomatic. Among them, 24 cases (35.8%) had gastric IFPs, 18 (27%) had colonic IFPs, 5 (7.5%) had rectal IFPs, 1 (1.5%) had a small intestinal IFP, and 1 (1.5%) had an esophageal IFP. Six patients (9%) presented to the emergency department with intestinal obstruction, all of whom had small intestinal IFPs. Three patients (4.5%) were diagnosed due to iron deficiency anemia, exclusively in those with gastric lesions. Upper gastrointestinal bleeding was observed in one patient (1.5%) with a gastric IFP, while lower gastrointestinal bleeding occurred in one patient (1.5%) with a colonic IFP. Additionally, nine patients (13.4%) reported nonspecific gastrointestinal symptoms, including dyspepsia, diarrhea, or early satiety, affecting five patients (7.5%) with gastric IFPs, two patients (3%) with colonic IFPs, one patient (1.5%) with a small intestinal IFP, and one patient (1.5%) with a rectal IFP. The relationship between symptoms and tumor location is detailed in Table 3.
Among the 32 patients with gastric IFP, 29 patients had chronic gastritis in the histological examination (87.9%) and Helicobacter pylori was present in 6 patients (18.2%). In line with the hypothesis of an inflammatory origin, no signs of macroscopic or microscopic chronic inflammation were observed in IFP localized in esophagus or rectum. Regarding colonic IFP, only one case exhibited microscopic evidence of indeterminate chronic inflammation.
The median tumor size was 1.67 cm (range 0.2–14 cm). While most inflammatory fibroid polyps are small, one case in our study involved a tumor reaching 14 cm in the colon. The IFP in the esophagus and rectum measured 0.6 cm, while those in the stomach and colon had a median size of 1.6 cm. In contrast, tumors in the small intestine were generally larger, with a median of 3.4 cm. All patients had a single tumor except for one (1.5%), who required a second surgery due the presence of another suspicious tumor in the small intestine.

3.3. Diagnostic Methods and Treatment

The diagnosis was primarily established through endoscopy, accounting for 57 cases (85.1%). CT was employed in seven patients (10.4%) and diagnosis was confirmed postoperatively in three cases (4.5%). Emergency diagnosis was defined as cases in which patients presented to the emergency department with acute symptoms directly related to the tumor, leading to its identification. A total of six patients (9%) were diagnosed in an emergency setting, all of whom presented with intestinal obstruction due to small bowel IFPs.
Vanek’s tumors were successfully resected endoscopically in 52 patients (77.6%), whereas surgical intervention was necessary for 15 patients (22.4%). Among those who underwent endoscopic resection, 26 patients (50%) had gastric IFP, 20 (38.4%) had colonic IFP, 5 (9.6%) in the rectum, and 1 patient (2%) had an esophageal lesion. In contrast, surgical treatment was performed in seven cases (46.7%) with IFP localized in small intestine, six in the stomach (40%), and two in the colon (13.3%). Urgent surgery was required in six patients (40% of all surgical cases), all of whom had tumors located in the small intestine. Notably, intestinal obstruction was the indication for surgery in these cases, accounting for 85% of all IFPs found in the small intestine. Clear resection margins were obtained in all cases, ensuring complete tumor removal. All data are summarized in Table 4.

3.4. Follow-Up and Recurrence

The median follow-up was 68.3 months (range from 11 to 136 months), and no recurrence was observed in any case. Additional information about patients and tumor characteristics are outlined in Table 5.

3.5. Statistical Analysis

3.5.1. Association Between Tumor Location and Treatment

A statistically significant association (p < 0.05) between tumor location and treatment was observed, with Cramér’s V = 0.65 indicating a strong association. While Vanek’s tumor in the stomach or colon is often managed by endoscopic resection, small intestine IFPs are more prone to need a surgical procedure.

3.5.2. Association Between Tumor Size and Treatment

Regarding tumor size and treatment, a significant association is also observed (p < 0.05). Larger tumor size correlates with an increased probability of requiring surgery, with a moderate effect size (Cohen’s r = 0.47).

3.5.3. Association Between Diagnosis and Treatment

Concerning emergency diagnosis, a significant association (p < 0.05) is found with the need of surgical treatment, demonstrating a moderate association (Cramér’s V = 0.459). Additionally, there is a strong association (Cramér’s V = 0.81) between emergency diagnosis and clinical manifestations.

3.5.4. Association Between Tumor Location and Diagnosis

Finally, a significant and a strong association (Cramér’s V = 0.75) is found between emergency diagnosis and location (p < 0.05). The small intestine is the most frequent location in the emergency setting; it is usually associated with intestinal obstruction due to intussusception.
All statistical associations and their corresponding p-values are summarized in Table 6.

4. Discussion

To our knowledge, this study includes the largest cohort of IFP cases reported in the scientific literature to date, with a total of 67 patients. Our results are mainly consistent with previous studies regarding location, symptoms, diagnosis, and treatment. Additionally, we have performed a detailed statistical analysis that offers a better understanding of this rare entity [4,22,24].
Our study concurs that Vanek’s tumor predominantly affects individuals in the fifth to seventh decades of life, with a median age of 60 years. There is a slight female predominance, according to our results. This is congruent with the epidemiological data reported in the most recent literature reviews [4,22,23,24,25].
Although etiology remains uncertain, different theories have been proposed: a reactive inflammatory response (associated mainly with Helicobacter pylori), an allergic reaction, or an autoimmune process [2,4]. In addition, some cases have been associated with Crohn’s disease, suggesting a potential association with inflammatory bowel conditions [26,27,28]. Chronic gastritis was observed in nearly 90% of cases, supporting the hypothesis that Vanek’s tumor may arise as a result of a reactive inflammatory process [2,4,29]. In non-gastric locations, we did not identify signs of chronic inflammation in the surrounding tissue, with the exception of one case in the colon. H. pylori was present in only 18% of cases, which is substantially lower than the general prevalence of H. pylori infection in Spain, which is approximately 40%, according to a seroprevalence study [30]. This disparity suggests that H. pylori infection may not represent a significant risk factor for IFP development.
The most common location for IFP is the stomach. Although other articles report the small intestine as the second most frequent site, our study indicates that the colon is the second most frequent location [4]. This discrepancy may be explained by the high frequency of colorectal cancer screening conducted in our environment, as well as the fact that most relevant literature reviews are focused on IFP causing intestinal intussusception [23,24].
In terms of clinical presentation, our data underscore the variable symptomatology of IFP. In contrast to other studies where pain is the most common symptom, our findings demonstrate that most patients are asymptomatic [4,24]. Screening endoscopies could also explain this difference. However, when symptoms do occur, nonspecific gastrointestinal symptoms and intestinal obstruction are the most prevalent, whereas gastrointestinal bleeding remains rare. Additionally, a strong association was identified between emergency diagnoses, clinical manifestations, and tumor location. This correlation confirms that patients presenting in urgent care settings exhibit a substantially higher likelihood of manifesting obstructive symptoms (predominantly resulting from intussusception).
Regarding treatment, the majority of IFPs in our study were successfully managed endoscopically (77.6%), particularly in gastric and colonic locations. Other studies report a wide range of percentages for endoscopic resection which vary from 20 to 60% [4,22,25]. Based on our data, gastric tumors are often successfully managed with endoscopic procedures, whereas small intestine tumors are more inclined to require surgical intervention due to intestinal obstruction. In fact, 85% of IFPs located in the small intestine needed urgent surgery. Advances in endoscopic techniques such as endoscopic mucosal resection (EMR) have broadened the range of lesions amenable to non-surgical removal. EMR is generally reserved for cases in which standard snare polypectomy may be insufficient, such as larger lesions or sessile polyps, where achieving complete resection requires a more advanced technique [18,31,32].
The primary challenge associated with small intestine involvement is the difficulty in achieving an early diagnosis due to the low precision of CT and the limited accessibility of this region to endoscopy. Consequently, these tumors often remain undetected until patients develop symptoms.
Our analysis further suggests that larger tumor size and emergency diagnosis have a moderate association with the requirement of surgical intervention. Indeed, all patients who presented in the emergency department needed an urgent surgery. In case of intestinal intussusception, management can be approached either by en bloc resection or reduction followed by resection. En bloc resection is strongly recommended in case of ileo-colic intussusception or when there is a high suspicion of malignancy. For small intestine intussusception, reduction followed by resection may be advisable when it can be performed safely [24,33,34].
The prognosis following complete removal of IFP is excellent, with a negligible risk of recurrence based on our data and only a single case of recurrence reported in the literature. Hence, long-term follow-up is generally not required after confirmed complete excision [35].
Some limitations should be considered in this analysis of IFPs. This retrospective study is inherently limited by selection and information biases. Our analysis was restricted to patients with symptomatic presentations or incidental endoscopic findings, potentially leading to an underdiagnosis of IFP in those who did not seek medical attention or underwent screening. The multicenter nature introduces variability between centers, which may reduce the precision of results. However, this multicenter design also enhances the external validity of the findings, making them more applicable to the broader population. Despite these limitations, the study provides valuable insights into these rare polyps, contributing significantly to the understanding of their characteristics and management.

5. Conclusions

This study provides the largest multicentric cohort of Vanek’s tumor cases to date, reinforcing the understanding of its clinical presentation, diagnostic challenges, and treatment outcomes. Our findings highlight the efficacy of endoscopic management, especially for gastric and colonic tumors, while underscoring the need for surgical intervention in small intestine cases. Prognosis after complete resection is excellent due to its benign nature, with only one recurrence reported in the literature. These results contribute significantly to the management and decision-making of Vanek’s tumors.

Author Contributions

Conceptualization: M.M.S. and V.D.-P.; methodology: M.M.S., V.D.-P., S.Q.Z. and P.V.C.; software: M.M.S.; validation: M.M.S., V.D.-P., S.Q.Z., H.D.Q.A., M.B.Á.Á., M.J.F., S.J.-G., H.G.L., D.G.O. and P.V.C.; formal analysis: M.M.S., V.D.-P., S.Q.Z., H.D.Q.A., M.B.Á.Á., M.J.F., C.M., H.G.L., D.G.O. and P.V.C.; investigation: M.M.S., V.D.-P., S.Q.Z., H.D.Q.A., M.B.Á.Á. and P.V.C.; resources: M.M.S., V.D.-P., S.J.-G., H.D.Q.A., M.B.Á.Á. and M.J.F.; data curation: M.M.S., V.D.-P., S.J.-G., H.D.Q.A., M.B.Á.Á. and M.J.F.; writing—original draft preparation: M.M.S. and P.V.C.; writing—review and editing: M.M.S., V.D.-P., S.Q.Z., S.J.-G., H.D.Q.A., M.B.Á.Á., M.J.F., C.M., H.G.L., D.G.O. and P.V.C.; visualization: M.M.S., V.D.-P., S.Q.Z. and P.V.C., Supervision., H.G.L., D.G.O. and P.V.C. Project administrator: M.M.S. and V.D.-P. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

This study received approval from Fundación Jiménez Díaz Hospital’s Ethics Committee. This approval was valid for all the hospitals involved (Hospital Universitario Fundación Jiménez Díaz, Hospital Universitario Rey Juan Carlos, Hospital Universitario General de Villalba, and Hospital Universitario Infanta Elena). The study follows the principles of the Declaration of Helsinki.

Informed Consent Statement

Informed consent was not required due to its retrospective nature.

Data Availability Statement

The data presented in this study is available on request from the corresponding author. The data are not publicly available due to ethical restrictions.

Conflicts of Interest

The authors declare no conflicts of interest.

Abbreviations

The following abbreviations are used in this manuscript:
CTComputer Tomography
EMREndoscopic Mucosal Resection
GI Gastrointestinal
GISTGastrointestinal Stromal Tumor
IFP Inflammatory fibroid polyp
KSKolmogorov–Smirnov
MRIMagnetic Resonance Imaging
PDGFRAPlatelet-Derived Growth Factor Receptor Alpha

References

  1. Vanek, J. Gastric Submucosal Granuloma with Eosinophilic Infiltration. Am. J. Pathol. 1949, 25, 397. [Google Scholar] [PubMed]
  2. Abboud, B. Vanek’s tumor of the small bowel in adults. World J. Gastroenterol. WJG 2015, 21, 4802. [Google Scholar] [CrossRef]
  3. Roseau, G.; Ducreux, M.; Molas, G.; Ponsot, P.; Amouyal, P.; Palazzo, L.; Amouyal, G.; Paolaggi, J.A. Epithelial gastric polyps in a series of 13000 gastroscopies. Presse Méd. 1990, 19, 650–654. [Google Scholar]
  4. Garmpis, N.; Damaskos, C.; Garmpi, A.; Georgakopoulou, V.E.; Sakellariou, S.; Liakea, A.; Schizas, D.; Diamantis, E.; Farmaki, P.; Voutyritsa, E. Inflammatory Fibroid Polyp of the Gastrointestinal Tract: A Systematic Review for a Benign Tumor. In Vivo 2021, 35, 81–93. [Google Scholar] [CrossRef]
  5. Kim, M.-K.; Higgins, J.; Cho, E.-Y.; Ko, Y.-H.; Oh, Y.L. Expression of CD34, bcl-2, and kit in inflammatory fibroid polyps of the gastrointestinal tract. Appl. Immunohistochem. Mol. Morphol. 2000, 8, 147–153. [Google Scholar] [CrossRef]
  6. Hasegawa, T.; Yang, P.; Kagawa, N.; Hirose, T.; Sano, T. CD34 expression by inflammatory fibroid polyps of the stomach. Mod. Pathol. 1997, 10, 451–456. [Google Scholar] [PubMed]
  7. Pappou, E.P.; Ahuja, N. The Role of Oncogenes in Gastrointestinal Cancer. Gastrointest. Cancer Res. 2010, S1, S2–S15. [Google Scholar]
  8. Schildhaus, H.U.; Caviar, T.; Binot, E.; Büttner, R.; Wardelmann, E.; Merkelbach-Bruse, S. Inflammatory fibroid polyps harbour mutations in the platelet-derived growth factor receptor alpha (PDGFRA) gene. J. Pathol. 2008, 216, 176–182. [Google Scholar] [CrossRef] [PubMed]
  9. Bjerkehagen, B.; Aaberg, K.; Steigen, S.E. Do Not Be Fooled by Fancy Mutations: Inflammatory Fibroid Polyps Can Harbor Mutations Similar to Those Found in GIST. Case Rep. Med. 2013, 2013, 845801. [Google Scholar] [CrossRef]
  10. Domínguez Prieto, V.; Camacho Aroca, A.; Calcerrada Alises, E. Intestinal intussusception due to Vanek’s tumour: A rare cause of intestinal obstruction in adults. Gastroenterol. Hepatol. 2023, 46, 560–561. [Google Scholar] [CrossRef]
  11. Santander, P.; Bush, A.; Kramer, N.; McCarthy, J. Running for the runs: Intermittent intussusception from Vanek tumor manifesting as constipation improved with exercise. Mil. Med. 2023, 188, e1314–e1315. [Google Scholar] [CrossRef]
  12. Hehir, C.; Calpin, G.; Dowling, G.; Spillane, C.; Kilgallen, C.; Hill, A.D.K. Inflammatory fibroid polyp of the small intestine presenting as small bowel obstruction with intussusception: A case report. J. Surg. Case Rep. 2024, 2024, rjad695. [Google Scholar] [CrossRef]
  13. Abu-Salah, A.K.; Brocken, E.; Mesa, H.; Collins, K. Jejunal intussusception secondary to a large inflammatory fibroid polyp: A case report and discussion of differential diagnosis. Case Rep. Pathol. 2023, 2023, 9417141. [Google Scholar] [CrossRef] [PubMed]
  14. Domínguez-Prieto, V.; León-Arellano, M.; Guadalajara, H.; García-Olmo, D. Vanek’s tumor: A differential diagnosis of colorectal cancer. Med. Clin. 2024, 163, e83. [Google Scholar] [CrossRef] [PubMed]
  15. Dagistanli, S.; Gunduz, N.; Sibic, O.; Sonmez, S. A rare cause of colonic obstruction: Inflammatory fibroid polyp. Cureus 2022, 14, e23868. [Google Scholar] [CrossRef]
  16. Shaib, Y.H.; Rugge, M.; Graham, D.Y.; Genta, R.M. Management of gastric polyps: An endoscopy-based approach. Clin. Gastroenterol. Hepatol. 2013, 11, 1374–1384. [Google Scholar] [CrossRef]
  17. Bechara, R.; Hurlbut, D.; Grin, A. Gastric inflammatory fibroid polyp: A rare incidental finding on endoscopy. J. Can. Assoc. Gastroenterol. 2021, 4, 149–150. [Google Scholar] [CrossRef] [PubMed]
  18. Matsubara, Y.; Tsuboi, A.; Hirata, I.; Sumioka, A.; Tanaka, H.; Yamashita, K.; Urabe, Y.; Oka, S. Gel immersion EMR of small-bowel inflammatory fibroid polyp using double-balloon endoscopy. VideoGIE 2024, 9, 92–94. [Google Scholar] [CrossRef]
  19. Obregón-Reyna, R.; Zapata-Martínez, M.Á.; Otero-Rodríguez, R.; Alanís-Rodríguez, O.C.; Garmendia-Cárdenas, G.; García-Cantú, A.J. Management of complicated inflammatory fibroid polyp by partial laparoscopic esophagogastrectomy—A case report. Cirugía Cir. 2020, 88, 5–8. [Google Scholar] [CrossRef]
  20. Kang, S.I.; Gu, M.J. Synchronous ileal inflammatory fibroid polyp and Meckel’s diverticulum found during laparoscopic surgery for adult intussusception. Yeungnam Univ. J. Med. 2020, 37, 226–229. [Google Scholar] [CrossRef]
  21. Moyón, F.X.; Molina, G.A.; Romero, K.; Moyón, M.A.; Cardenas, B.A.; Tufiño, J.; Almeida, M.B.; González, H.R.; Moyon, P. Laparoscopy and intraoperative enteroscopy, a helpful tool in a rare tumor (inflammatory fibroid polyp) of the small bowel. A case report. Ann. Med. Surg. 2021, 66, 102355. [Google Scholar] [CrossRef] [PubMed]
  22. Inayat, F.; Ur Rahman, A.; Wahab, A.; Riaz, A.; Zahid, E.; Bejarano, P.; Pimentel, R. Gastric inflammatory fibroid polyp: A rare cause of occult upper gastrointestinal bleeding. J. Investig. Med. High Impact Case Rep. 2020, 8, 2324709620936840. [Google Scholar] [CrossRef] [PubMed]
  23. Ivaniš, N.; Tomas, V.; Vranić, L.; Lovasić, F.; Ivaniš, V.; Žulj, M.; Šuke, R.; Štimac, D. Inflammatory fibroid polyp of the small intestine: A case report and systematic literature review. J. Gastrointest. Liver Dis. 2020, 29, 455–460. [Google Scholar] [CrossRef]
  24. Kao, Y.-K.; Chen, J.-H. Adult Jejuno-jejunal intussusception due to inflammatory fibroid polyp: A case report and literature review. Medicine 2020, 99, e22080. [Google Scholar] [CrossRef]
  25. Wang, J.; Tian, X.; Ning, B.F.; Wang, X.H.; Yuan, Z.L.; Li, B.B.; Shi, B.; Xie, W.F. Clinical characteristics and prognosis of inflammatory fibroid polyp in the gastrointestinal tract: A series of nine cases and a literature review. J. Dig. Dis. 2020, 21, 737–740. [Google Scholar] [CrossRef] [PubMed]
  26. Theodoropoulos, G.E.; Linardoutsos, D.; Tsamis, D.; Stamopoulos, P.; Giannopoulos, D.; Zagouri, F.; Michalopoulos, N.V. Gastrointestinal stromal tumor causing small bowel intussusception in a patient with Crohn’s disease. World J. Gastroenterol. WJG 2009, 15, 5224. [Google Scholar] [CrossRef]
  27. Deschamps, L.; Bretagnol, F.; Couvelard, A.; Corcos, O.; Bedossa, P.; Panis, Y. Inflammatory fibroid polyp in Crohn’s disease revealed by ileoileal intussusception: Case report and review of the literature. Inflamm. Bowel Dis. 2008, 14, 1317–1320. [Google Scholar] [CrossRef]
  28. Parasi, A.; Triantafillidis, J.K.; Barbatzas, C.; Karakosta, A.; Condilis, N.; Sotiriou, H. Coexistence of Crohn’s disease and inflammatory fibroid polyp of the small bowel. Rep. A Case Rev. Lit. 2005, 76, 395–399. [Google Scholar]
  29. Kawai, A.; Matsumoto, H.; Haruma, K.; Kanzaki, T.; Sugawara, Y.; Akiyama, T.; Hirai, T. Rare case of gastric inflammatory fibroid polyp located at the fornix of the stomach and mimicking gastric cancer: A case report. Surg. Case Rep. 2020, 6, 292. [Google Scholar] [CrossRef]
  30. Caldas, M. Registro Español de Helicobacter Pylori: Análisis de los datos Españoles Incluidos En El Registro Europeo de H. Pylori (Hp-EuReg); Universidad Autónoma de Madrid: Madrid, Spain, 2019. [Google Scholar]
  31. Wang, X.; Ma, R.; Ma, J.; Tang, N.; Li, R.; Ma, X. Endoscopic submucosal dissection for the treatment of a large inflammatory fibroid polyp in the gastric antrum prolapsing into the duodenum: A case report. Medicine 2024, 103, e37877. [Google Scholar] [CrossRef]
  32. Rizzi, F.; Sacco, M.; Debernardi Venon, W.; Trinh, D.A.A.; Pennazio, M. A transvalvular polypectomy of a giant ileal inflammatory fibroid polyp by retrograde single-balloon enteroscopy. Endoscopy 2022, 54, E526–E527. [Google Scholar] [CrossRef] [PubMed]
  33. Rollo, A.; Lugani, P.; Casali, L.; Montali, F.; Scaramuzza, L.; Gandolfi, G.; Thai, E.; Costi, R. Intussusception of the bowel in adult women due to bulky inflammatory fibroid polyp treated in emergency. A case report. Acta Biomed. 2022, 93, e2022117. [Google Scholar] [CrossRef]
  34. Gadoura, A.; Mohammed, F.; Abdulkarim, M.; Ibn Yasir, A.; Shani, D.; Salih, N. Inflammatory fibroid polyp (Vanek’s tumor) causing double compound ileo-ileal intussusception in an adult patient, a case report. Int. J. Surg. Case Rep. 2022, 93, 106947. [Google Scholar] [CrossRef] [PubMed]
  35. Zinkiewicz, K.; Zgodzinski, W.; Dabrowski, A.; Szumilo, J.; Cwik, G.; Wallner, G. Recurrent inflammatory fibroid polyp of cardia: A case report. World J. Gastroenterol. 2004, 10, 767–768. [Google Scholar]
Table 1. Vanek’s tumor locations along the GI tract.
Table 1. Vanek’s tumor locations along the GI tract.
LocationTotal
Stomach3247.8%
Antrum25(78.1% of gastric tumors)
Corpus4(12.5% of gastric tumors)
Pylorus3(9.4% of gastric tumors)
Colon2232.8%
Left colon17(77.3% of colonic tumors)
Right colon3(13.6% of colonic tumors)
Transverse colon2(9.1% of colonic tumors)
Small intestine710.4%
Rectum57.5%
Esophagus11.5%
Table 2. Distribution of tumor locations by sex and mean age.
Table 2. Distribution of tumor locations by sex and mean age.
LocationMaleFemaleMean Age
Esophagus1 (3.6%)0 (0%)57
Stomach12 (42.9%)20 (51.3%)63
Small intestine2 (7.1%)5 (12.8%)55
Colon9 (32.1%)13 (33.3%)59
Rectum4 (14.3%)1 (2.6%)56
Total28 (100%)39 (100%)
Table 3. Locations and clinical manifestations of IFP.
Table 3. Locations and clinical manifestations of IFP.
EsophagusStomachSmall IntestineColonRectum
Asymptomatic1 (1.5%)24 (35.8%)1 (1.5%)18 (27%)5 (7.5%)
Upper GI bleeding0 (0%)1 (1.5%)0 (0%)0 (0%)0 (0%)
Lower GI bleeding0 (0%)0 (0%)0 (0%)2 (3%)0 (0%)
Anemia0 (0%)3 (4.5%)0 (0%)0 (0%)0 (0%)
Intestinal obstruction0 (0%)0 (0%)6 (9%)0 (0%)0 (0%)
Nonspecific symptoms0 (0%)4 (6%)0 (0%)2 (3%)0 (0%)
Table 4. Locations and treatment of IFP.
Table 4. Locations and treatment of IFP.
LocationEndoscopy Resection Surgical Procedure
Esophagus1/1 (100%)0/1 (0%)
Stomach26/32 (81.3%)6/32 (18.7%)
Small intestine 0/7 (0%)7/7 (100%)
Colon 20/22 (90.9%)2/22 (9.1%)
Rectum5/5 (100%)0/5 (0%)
Table 5. Patients and tumor characteristics.
Table 5. Patients and tumor characteristics.
Variable Total (n = 67)
Age (years)60 (32–83)
SexFemale: 39 (58.2%)
Male: 28 (41.8%)
Clinical manifestationsAsymptomatic: 49 (73.1%)
Upper GI bleeding: 1 (1.5%)
Lower GI bleeding: 2 (3%)
Anemia: 3 (4.5%)
Obstruction: 6 (9%)
Nonspecific symptoms: 6 (9%)
Helicobacter pylori6 (18.2% of gastric tumor)
Chronic gastritis29 (87.9% of gastric tumor)
Unique tumor66 (98.5%)
Tumor size (cm)1.67 (range 0.2–14)
DiagnosisEndoscopy: 57 (85.1%)
CT: 7 (10.4%)
Surgery: 3 (4.5%)
Emergency diagnosis6 (9%)
Treatment Endoscopic resection: 52 (77.4%).
Surgical treatment: 15 (22.4%)
Need of urgent treatment6 (9%)
Recurrence 0 (0%)
Follow-up time (months)68.3 (11–136)
Table 6. Statistical associations.
Table 6. Statistical associations.
Associations p-Value
Tumor location and sexp = 0.282
Tumor location and age p = 0.488
Tumor location and treatment p < 0.05
Tumor size and treatmentp < 0.05
Diagnosis and treatmentp < 0.05
Tumor location and diagnosis p < 0.05
Disclaimer/Publisher’s Note: The statements, opinions and data contained in all publications are solely those of the individual author(s) and contributor(s) and not of MDPI and/or the editor(s). MDPI and/or the editor(s) disclaim responsibility for any injury to people or property resulting from any ideas, methods, instructions or products referred to in the content.

Share and Cite

MDPI and ACS Style

Sánchez, M.M.; Domínguez-Prieto, V.; Qian Zhang, S.; Quiceno Arias, H.D.; Álvarez Álvarez, M.B.; Fuertes, M.J.; Meliga, C.; Jiménez-Galanes, S.; Labajo, H.G.; Olmo, D.G.; et al. Inflammatory Fibroid Polyp (Vanek’s Tumor): A Retrospective Multicentric Analysis of 67 Cases. Cancers 2025, 17, 1209. https://doi.org/10.3390/cancers17071209

AMA Style

Sánchez MM, Domínguez-Prieto V, Qian Zhang S, Quiceno Arias HD, Álvarez Álvarez MB, Fuertes MJ, Meliga C, Jiménez-Galanes S, Labajo HG, Olmo DG, et al. Inflammatory Fibroid Polyp (Vanek’s Tumor): A Retrospective Multicentric Analysis of 67 Cases. Cancers. 2025; 17(7):1209. https://doi.org/10.3390/cancers17071209

Chicago/Turabian Style

Sánchez, Mario Martín, Víctor Domínguez-Prieto, Siyuan Qian Zhang, Hernán Darío Quiceno Arias, María Bernarda Álvarez Álvarez, Montiel Jiménez Fuertes, Cecilia Meliga, Santos Jiménez-Galanes, Héctor Guadalajara Labajo, Damián García Olmo, and et al. 2025. "Inflammatory Fibroid Polyp (Vanek’s Tumor): A Retrospective Multicentric Analysis of 67 Cases" Cancers 17, no. 7: 1209. https://doi.org/10.3390/cancers17071209

APA Style

Sánchez, M. M., Domínguez-Prieto, V., Qian Zhang, S., Quiceno Arias, H. D., Álvarez Álvarez, M. B., Fuertes, M. J., Meliga, C., Jiménez-Galanes, S., Labajo, H. G., Olmo, D. G., & Campos, P. V. (2025). Inflammatory Fibroid Polyp (Vanek’s Tumor): A Retrospective Multicentric Analysis of 67 Cases. Cancers, 17(7), 1209. https://doi.org/10.3390/cancers17071209

Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.

Article Metrics

Back to TopTop