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Intest Res > Volume 20(2); 2022 > Article
Kedia, Sharma, Vuyyuru, Madhu, Sahu, Kante, Das, Goyal, Madan, Makharia, and Ahuja: Addition of computed tomography chest increases the diagnosis rate in patients with suspected intestinal tuberculosis

Abstract

Background/Aims

Intestinal tuberculosis (ITB) is difficult to diagnose due to poor sensitivity of definitive diagnostic tests. ITB may be associated with concomitant pulmonary tuberculosis (PTB) which may remain undetected on chest X-ray. We assessed the role of contrast enhanced computed tomography (CECT) chest in detecting the prevalence of active PTB, and increasing the diagnostic yield in patients with suspected ITB.

Methods

Consecutive treatment naïve patients with suspected ITB (n=200) who underwent CECT chest (n=88) and had follow-up duration>1 year were recruited in this retrospective study (February 2016 to October 2018). ITB was diagnosed in the presence of caseating granuloma, positive acid fast stain or culture for Mycobacterium tuberculosis on biopsy, presence of necrotic lymph nodes (LNs) on CT enterography or positive response to anti-tubercular therapy. Evidence of active tuberculosis on CECT-chest was defined as presence of centrilobular nodules with or without consolidation/miliary nodules/thick-walled cavity/enlarged necrotic mediastinal LNs.

Results

Sixty-five of eighty-eight patients (mean age, 33.8±12.8 years; 47.7% of females) were finally diagnosed as ITB (4-caseating granuloma on biopsy, 12-necrotic LNs on CT enterography, 1-both, and 48-response to anti-tubercular therapy) and 23 were diagnosed as Crohn’s disease. Findings of active TB on CECT chest with or without necrotic abdominal LNs were demonstrated in 5 and 20 patients, respectively. No patient with Crohn’s disease had necrotic abdominal LNs or active PTB. Addition of CECT chest in the diagnostic algorithm improved the sensitivity of ITB diagnosis from 26.2% to 56.9%.

Conclusions

Addition of CECT chest significantly improves the sensitivity for definite diagnosis in a patient with suspected ITB.

INTRODUCTION

Ever since the diagnostic criteria for intestinal tuberculosis (ITB) were laid down by Logan in 1964 [1], there have been minimal reforms in these criteria, and in lieu of the poor sensitivity of these criteria, the diagnosis of ITB remains a challenge. This problem is further compounded by the increasing disease burden of Crohn’s disease (CD), a close mimicker of ITB [2]. Because of poor sensitivity of diagnostic techniques for ITB and lack of specificity for diagnostic criteria for CD, differentiating CD and ITB remains challenging, and this dilemma is often resolved by a therapeutic anti-tubercular therapy (ATT) trial [3]. However, this therapeutic ATT trial is associated with the risk of ATT induced adverse events, notably hepatotoxicity, delay in the diagnosis of CD, and as recently demonstrated by us, complicated course of patients eventually diagnosed with CD [4]. Hence there is a constant need for improvement in diagnostic strategies for ITB.
Up to one-fourth of patients with ITB have evidence of old/active TB on simultaneous chest X-ray [5]. Contrast enhanced computed tomography (CECT) chest has better sensitivity than chest X-ray to detect parenchymal as well/mediastinal lesions suggestive of active TB [6-8]. CECT chest, if done in patients with suspected ITB, would help in classifying the disease accurately at the outset itself as ITB. This would also increase the confidence of clinicians in starting ATT in a patient with suspected ITB.
The present study was therefore aimed to evaluate the role of CECT chest during the initial workup of ITB.

METHODS

1. Patients

Consecutive patients with suspected ITB followed up at the Department of Gastroenterology at the All India Institute of Medical Sciences, New Delhi, India from February 2016 to October 2018 were screened for inclusion in the study. The patients were included if they underwent CECT chest prior to starting ATT, remained on regular follow-up (at least 1 year after ATT) and had repeat evaluation for endoscopic/radiologic healing after completion of ATT. Permission from the Institute Ethics Committee of All India Institute of Medical Sciences was obtained (IEC-52/04.01.2019) and the informed consent was waived.

2. Study Design

This retrospective analysis of a prospectively maintained database screened 200 consecutive patients with suspected diagnosis of ITB of which 88 underwent CECT of chest before ATT was started and had a follow-up of 1 year after ATT. At our center, all patients with suspected ITB are subjected to a uniform evaluation including baseline complete blood count, liver function tests, renal function tests, chest X-ray, cross-sectional imaging (computed tomography/magnetic resonance [CT/MR] enterography), endoscopy (upper gastrointestinal endoscopy/ileocolonoscopy according to suspected site of involvement) and biopsy for histopathological examination, acid fast bacillus (AFB), culture and polymerase chain reaction for Mycobacterium tuberculosis. CT/MR enterography is done according to a predefined protocol followed at our center. In addition, a CECT chest was also done for these patients. The data was compiled on a predefined proforma on demographics, mode of diagnosis of ITB, disease duration, clinical, endoscopic, histologic and radiologic features, clinical and radiologic/endoscopic response to ATT.

3. Diagnosis of ITB

The diagnosis of ITB was made in an appropriate clinical setting with the demonstration of necrotizing granulomas on histopathology, demonstration of AFB on histopathology or culture of intestinal tissue, and presence of necrotic lymph nodes on CT enterography (CTE) [1,9]. In patients who did not fulfill the above definitions, therapeutic trial with ATT was given. Diagnosis of ITB was made if patient had clinical and endoscopic/radiologic response to ATT after completion of ATT at 6 to 9 months. These defining criteria for diagnosis of ITB have been validated earlier in another study at our center. In patients not responding to ATT, response to CD specific therapy confirmed the diagnosis of CD [3].

4. Treatment and Follow-up

Induction regimen of isoniazid 5 mg/kg, rifampicin 10 mg/kg, pyrazinamide 20-25 mg/kg and ethambutol 15-20 mg/kg for 2 months followed by maintenance therapy of isoniazid and rifampicin for duration of 4-7 months was given. The total treatment duration was 6-9 months depending upon the response to ATT. Patients were routinely followed up at 2 monthly intervals and as and when required to assess symptom response and also to monitor drug toxicity by assessment of liver function tests. Repeat endoscopy/cross-sectional imaging were done to assess mucosal healing (on endoscopy) or radiologic resolution.

5. Definitions

(1) Ulceroconstrictive disease: gastrointestinal disease which occurs due to ulcers or stricture in the small or large intestine; (2) Suspected ITB: patients with ulceroconstrictive intestinal disease with clinical/endoscopic/radiologic features suggestive of ITB; (3) Definite ITB: patients with suspected ITB who fulfilled the diagnostic criteria for ITB; (4) Indeterminate ITB: patients with suspected ITB who did not fulfill the diagnostic criteria for ITB; (5) Mucosal healing: mucosal healing was defined as absence of any evidence of ulceration, erythema (suggestive of active inflammation) on follow-up colonoscopy. Radiologically absence of any signs of inflammatory stricture was also classified as mucosal healing; or (6) Active tuberculosis on CT chest: active tuberculosis on CT chest was defined in the presence of air-space nodules/centrilobular nodules/clustered nodules or consolidation in apical and posterior segments of right upper lobe, apicoposterior segment of left upper lobe/right middle lobe/lingula, and superior segment in any lower lobe, miliary nodules, thick-walled cavity, cavity with surrounding consolidation, enlarged mediastinal lymph nodes with central necrosis (rim enhancement) or heterogeneous enhancement [8].

6. Statistical Analysis

Continuous variables were expressed as median with interquartile range (IQR) or mean ± standard deviation, depending upon normal or non-normal distribution, and categorical variables were expressed as percentages. McNemar test of proportions was used to compare the sensitivity of definite ITB diagnosis with and without CT chest. SPSS software version 20.0 (IBM Corp., Armonk, NY, USA) and STATA software version 12 (StataCorp, College Station, TX, USA) was used for analysis.

RESULTS

A total of 200 treatment naïve patients with suspected ITB were evaluated between February 2016 till October 2018. Of these, 88 patients underwent CECT chest before ATT and had a follow-up of 1 year after ATT. Of these 88 patients, 65 were diagnosed with ITB and 23 were diagnosed with CD.

1. Baseline Demographic, Clinical, Endoscopic and Radiologic Characteristics

The mean age and median disease duration of patients with ITB were 33.8 ± 12.8 years and 12 months (IQR, 6-24 months) respectively. Thirty-four patients (52.3%) were males. The most common symptom was abdominal pain, seen in 92.3% of patients followed by weight loss (63.1%) and recurrent partial bowel obstruction (41.5%). Fever was present in 30.8% of patients (Table 1). On colonoscopy, caecum and terminal ileum was the most commonly involved site, seen in 40.0% and 51.2% patients respectively, and presence of transverse ulcer was the most common endoscopic feature, seen in 65.5% patients (Table 2). On histology, granulomas were seen in 39.6% patients, while caseation was seen in only 8.6% patients. The median granuloma size was 300 μm (IQR, 130-400 μm). Microgranuloma (< 200 μm) was present in 5 patients. On CTE, 43.1% of patients had evidence of stricture, 61.5% of patients had short segment involvement, mural stratification was seen in 36.9% of patients and evidence of necrotic lymph nodes was seen in 20% of patients (n = 13) (Fig. 1). Twenty-five patients had evidence of active tuberculosis on CT chest (Fig. 2), of which 18 had parenchymal lesions and 3 had evidence of necrotic lymph nodes and 4 had both findings (Table 3). Nineteen patients with ITB (29%) and 5 patients with CD (22%) had evidence of prior TB in the form of fibrotic lesions and calcified granulomas on CT chest.

2. Diagnostic Criteria for TB

Of 88 patients, 65 were diagnosed with ITB, of which 4 patients had evidence of caseating granulomas on biopsy, and 12 had presence of necrotic lymph nodes on CTE, and 1 had both, confirming the diagnosis of ITB. In rest of the patients, the diagnosis was confirmed on follow-up, with documentation of clinical and endoscopic/radiologic response. Therefore, 73.8% patients required therapeutic ATT trial. Of 13 patients with necrotic lymph nodes on CTE, imaging was repeated in 6, and 5 out of 6 patients showed resolution of these necrotic lymph nodes.
Twenty-three patients were eventually diagnosed as CD, because of non-response to ATT and improvement with CD specific therapy.

3. Role of CECT Chest in the Diagnosis of ITB

Of 65 patients with ITB, 20 patients had evidence of active tuberculosis on CT chest, and 5 had evidence of both necrotic lymph nodes on CTE and active TB on CECT chest, while none of the 23 patients with CD either had either evidence of active TB on CT chest or necrotic lymph nodes on CTE. Of 25 patients with positive CECT chest, only 1 was symptomatic for pulmonary TB. Bronchoalveolar lavage for AFB was done in 3 patients, and was positive in 1 patient. Repeat imaging done in 3 patients demonstrated complete healing of chest lesions with ATT.
Therefore, if CECT chest findings were included in the diagnostic criterion for ITB, then in the present study, patients who would be diagnosed with ITB at the onset would increase from 17 of 65 to 37 of 65, increasing the diagnostic sensitivity of available investigations (including CT findings) for ITB from 26.1% to 56.9%, which was statistically significant (P<0.001).

DISCUSSION

Abdominal tuberculosis is the sixth most common form of extrapulmonary tuberculosis (EPTB) [10], and ITB is the major manifestation of abdominal tuberculosis. Except for lymph node tuberculosis, diagnosing EPTB has always remained a challenge, primarily because of its paucibacillary nature, which makes it difficult to isolate the organism, the demonstration of which is a definite diagnostic criterion for any infectious disease. Caseation necrosis on biopsy, another pathognomonic hallmark of EPTB is again a rare entity [11], and therefore the sensitivity for diagnosis of EPTB/ITB has always remained low. Further, if the involvement in ITB is limited to small bowel only, then obtaining biopsy samples becomes difficult and these definitive microbiological/pathological tests cannot be applied. Presence of necrotic lymph nodes on CTE adds to the diagnostic accuracy, but this feature is also limited by poor sensitivity, as shown in a recent meta-analysis [12]. This diagnostic gap for EPTB has been circumvented by the so called composite reference standard which includes demonstration of clinical response to ATT after the therapeutic ATT trial. However, because of diagnostic confusion with CD and presence of ATT response in a proportion of patients with CD [3], the composite reference standard for ITB also includes the demonstration of endoscopic/radiologic response to ATT. However, the therapeutic trial with ATT is associated with the short-term risk of ATT induced hepatotoxicity, and as recently reported by us, long term risk of complicated disease course in patients eventually diagnosed with CD [4]. Hence, there is a need for better diagnostic modalities for upfront definite diagnosis of ITB [13-15]. One of these could be the demonstration of active tuberculosis at extraintestinal site, and the most common site would be pulmonary tuberculosis, as shown in the present study, where addition of CECT chest improved the sensitivity for diagnosing ITB.
Of 88 patients with suspected ITB, 65 were finally diagnosed with ITB, and in 73.8% of patients, the basis for diagnosis was therapeutic response to ATT. Of the definite diagnostic tests for ITB, caseating granulomas were positive in 5 patients, and necrotic lymph nodes on CT were present in 13 patients. These necrotic lymph nodes were not subjected to tissue diagnosis because the underlying clinical setting was strong for ITB, and 5 out of 6 patients in whom imaging was repeated, showed resolution of necrotic lymph nodes. Thus, overall sensitivity of ITB diagnosis was only 26.2%, which was is comparable to other series.
The most interesting finding of this study was the demonstration of active tuberculosis on CECT chest in 38.5% of patients with ITB, with only 1 patient being symptomatic for pulmonary TB. Recent guidelines on EPTB have suggested a chest X-ray in the diagnostic algorithm of a patient with suspected EPTB [16], and multiple series on ITB have demonstrated evidence of old/active TB on chest X-ray in up to 25% patients [5]. Further, multiple series on CD/ITB differentiation have suggested demonstration of active pulmonary TB in patients with ITB as the definite differentiating feature between the 2 conditions [17,18]. The present study has extended this observation by utilizing a more sensitive and a definitive diagnostic technique for detecting associated pulmonary lesions in patients with ITB.
Inclusion of positive CT chest findings as a definite diagnostic criterion significantly increased the sensitivity of diagnosing ITB, from 26% to 57%, which suggests for the inclusion of CT chest in the diagnostic algorithm of a patient with suspected ITB (Fig. 3). However, there is a risk of radiation with additional CTs, and we therefore suggest CT chest in patients where the definitive diagnostic criteria including necrotic lymph nodes are not met and the chest X-ray is inconclusive (Fig. 3). Presence of active TB on CT chest would increase the confidence in diagnosis of ITB and initiation of ATT. Patients who are initiated on ATT in the absence of these criteria (therapeutic ATT trial) need to be followed up vigilantly with early assessment for endoscopic/clinical response, as we have recently shown that ATT in patients with eventual diagnosis of CD predisposes to stricture formation [4].
The study is limited by its retrospective design and small sample size. However, the data was collected from a prospectively maintained database and included consecutive patients with suspected ITB who underwent CECT chest before ATT was administered and had a follow-up of more than 1 year. One year of follow-up ensured that the diagnosis of ITB was definite in those patients who were administered therapeutic ATT trial and sustained their response till 1 year. There was lack of histological/microbiological proof of TB either from necrotic lymph nodes or from CT chest. However, search for definite TB in this setting would involve invasive techniques, increase the time to diagnosis and because of their poor sensitivity, absence of definite evidence will not refute the diagnosis of ITB. Moreover, the diagnosis of active TB on CT chest was entertained after consulting pulmonologist and we could demonstrate radiological healing after ATT in a fraction of patients. The results also require validation in a large sample size from other centers.
Though, including only patients with suspected ITB could have biasedly increased the chance of positive findings on CT chest, the primary objective of this study was to evaluate the role of CT chest in increasing upfront diagnosis rate in patients with suspected ITB. Hence, the study provides a simple message that among patients with suspected ITB who do not fulfill the definitive diagnostic criteria for ITB, addition of CT chest might increase the physician’s confidence in the diagnosis of ITB in a particular patient. Moreover, absence of active TB on CT chest in patients who were eventually diagnosed with CD, further increases our confidence in the role of CT chest on this aspect.
To conclude, there is a significant improvement in diagnostic sensitivity with the addition of CECT chest findings in the diagnostic algorithm of a patient with suspected ITB.

ADDITIONAL INFORMATION

Funding Source

This study was supported by the Indian Council of Medical Research: Centre for advanced research and excellence in intestinal diseases (grant number: 55/4/11/CARE-ID/2018-NCD-II).

Conflict of Interest

No potential conflict of interest relevant to this article was reported.

Author Contribution

Conceptualization: Ahuja V. Data curation: Kedia S, Vuyyuru SK, Madhu D. Formal analysis: Kedia S, Vuyyuru SK, Goyal A. Investigation: Sharma R. Methodology: Goyal A, Ahuja V. Project administration, supervision: Ahuja V. Writing - original draft: Kedia S, Makharia G, Ahuja V. Writing - review & editing: Sharma R, Vuyyuru SK, Madhu D, Sahu P, Kante B, Das P, Goyal A, Madan K, Makharia G, Ahuja V. Approval of final manuscript: all authors.

Fig. 1.
(A, B) Axial computed tomography (CT) enterography images showing enlarged lymph nodes with central necrosis and peripheral enhancement in the pericolic region (white arrow) along with colonic thickening (black arrow). (C) Coronal reformatted CT enterography image showing inflammatory stricture in the ascending colon (white arrow).
ir-2020-00104f1.jpg
Fig. 2.
Axial contrast enhanced computed tomography (CECT) mediastinal window (A) and lung window (B) showing necrotic subcarinal lymph node (white arrow) and acinar nodules some of which show tree-in-bud morphology (black arrow). (C) Axial CECT abdomen with positive oral contrast showing thickening of ileal loops (white arrow) and few necrotic mesenteric lymph nodes (white arrowhead).
ir-2020-00104f2.jpg
Fig. 3.
Diagnostic algorithm in a patient with suspected ITB incorporating CT chest. aFeatures suggestive CD: (1) Clinical: diarrhea/perianal lesions/bleeding per-rectum; (2) Endoscopy: linear ulcers/cobblestoning; (3) CTE: skip lesions/comb sign/long segment involvement/increased visceral fat; or (4) Biomarker: low peripheral blood FOXP3 T regulatory cells. CD, Crohn’s disease; ITB, intestinal tuberculosis; HPE, histopathology; AFB, acid fast bacillus; MTB, Mycobacterium tuberculosis; CTE, computed tomography enterography; CECT, contrast enhanced computed tomography; TB, tuberculosis; ATT, anti-tubercular therapy.
ir-2020-00104f3.jpg
Table 1.
Clinical and Demographic Features of Patients with Intestinal Tuberculosis
Variable Intestinal tuberculosis (n = 65)
Age (yr) 33.8 ± 12.8
Female sex 31 (47.7)
Duration of symptoms (mo) 12 (6-24)
Fever 20 (30.8)
Diarrhea 14 (21.5)
Constipation 22 (33.8)
Gastrointestinal bleeding 9 (13.8)
Pain abdomen 60 (92.3)
Partial bowel obstruction 27 (41.5)
Weight loss 41 (63.1)
Anemia 45 (69.2)

Values are presented as mean±standard deviation, number (%), or median (interquartile range).

Table 2.
Endoscopic Features of Patients with Intestinal Tuberculosis
Variable Intestinal tuberculosis (n = 65)
Site of involvement
 Rectum 3/58 (5.2)
 Sigmoid colon 3/58 (5.2)
 Descending colon 3/58 (5.2)
 Transverse colon 9/58 (15.5)
 Ascending colon 14/57 (24.6)
 Caecum 20/50 (40.0)
 Terminal ileum 22/43 (51.2)
 Ileocecal valve 18/50 (36.0)
Type of involvement
 Aphthous ulcers 12/57 (21.1)
 Longitudinal ulcers 3/55 (5.5)
 Transverse ulcers 36/55 (65.5)
 Pseudopolyps 3/58 (5.2)
 Nodularity 6/58 (10.3)
 Stricture 19/58 (32.7)
Histology
 Granuloma 23/58 (39.6)
 Caseation 5/58 (8.6)

Values are presented as number/number (%).

Table 3.
CT Findings in Patients with ITB
Variable ITB (n = 65)
Site of involvement
 Left colona 1 (1.5)
 Colonb 8 (12.3)
 Ileocecal areac 32 (49.2)
 Rest of small intestined 20 (30.8)
Type of involvement
 Long segment involvement 25 (38.5)
 Asymmetric thickening 8 (12.3)
 Mural stratification 24 (36.9)
 Stricture 28 (43.1)
 Mesenteric changes 29 (44.6)
  Comb sign 13
  Fat proliferation 16
 Necrotic abdominal lymph nodes 13 (20.0)
 Active TB on CT chest 25 (38.5)
  Parenchymal lesions 18
  Necrotic mediastinal lymph nodes 3
  Both 4
 Active TB on CT chest in patients with definite TB (n = 17) 7 (41.2)
 Active TB on CT chest in patients without definite TB (n = 48) 18 (37.5)
P-value 0.79

Values are presented as number (%) or number.

a Left colon includes descending colon, sigmoid colon, rectum.

b Colon includes caecum (without contiguous terminal ileal involvement), ascending colon, transverse colon and left colon.

c Rest of small intestine includes jejunum, ileum excluding the terminal ileum.

d Ileocecal area includes terminal ileum just adjacent to the ileocecal valve or contiguous terminal ileal and cecal involvement.

TB, tuberculosis; ITB, intestinal tuberculosis; CT, computed tomography.

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