The diagnostic yield of closed needle pleural biopsy in exudative pleural effusion: a retrospective 10-year study

Introduction

A pleural effusion is defined as an abnormal accumulation of pleural fluid within the pleural space, commonly classified as either transudative or exudative (1), which can be differentiated by thoracocentesis and biochemical analysis. However, approximately 40% of exudative pleural effusion cannot be diagnosed by thoracocentesis, creating the need for pleural biopsy or thoracoscopy (2).

Closed pleural biopsy (CPB), which was first reported by De Francis in 1955, has become a common method of obtaining pleural tissue for the diagnosis of pleural diseases (3). Copes and Abrams’s needles were the most popular CPB needles after practical modification (4,5). CPB is a simpler and inexpensive technique that can be regularly carried out in hospitals at different levels. The complications of CPB mainly include pneumothorax, chest pain, vasovagal syncope, and hemothorax (6,7). Previous studies have demonstrated that while CPB has lower diagnostic accuracy, it also has lower rates of complications than thoracoscopy (8,9).

Thoracoscopy, with its high level of diagnostic accuracy, has been recognized as the gold standard for diagnosing pleural lesions (10). However, according to the results of different studies, the sensitivity of thoracoscopy is only approximately 90% to 95% (8,9). Therefore, CPB is still considered as an essential method to diagnose exudative pleural effusion owing to its practicability and safety in pleural diseases. This study was performed to assess the efficiency of CPB in the diagnosis of exudative pleural effusion at Nanjing Jinling Hospital and Nanjing Jiangning Hospital of China in the past decade.

Methods

This was a double-center retrospective study of patients with undiagnosed pleural effusion who underwent CPB (Figure 1) in Nanjing Jinling Hospital and Nanjing Jiangning Hospital in the ten-year period from January 01, 2008, to July 30, 2018. Thoracentesis and biochemical analyses were carried out for patients with unidentified pleural effusion. Light’s criteria were used to distinguished exudative from transudative pleural effusion. For unknown exudative pleural effusion, tuberculosis and malignancy were diagnosed as follows: (I) tuberculous pleural effusion (TPE) was diagnosed if one of the following applied: granuloma was found by histopathology; Ziehl-Neelsen acid-fast staining was positive; adenosine deaminase (ADA) in pleural effusion was higher than 35IU with clinical symptoms of TB or γ-interferon increased with symptoms of TB, or mycobacterium tuberculosis could be cultured from pleural effusion or pleural tissue; (II) malignant pleural effusion (MPE) was confirmed when histopathological evidence was obtained by pleural biopsy, pneumocentesis, fibrobronchoscopy, surgery, or pleural fluid cytology.

Figure 1 Pleural biopsy needle.

Results

Overall, a total of 730 patients with exudative pleural fluid who underwent CPB at Nanjing Jinling Hospital and Nanjing Jiangning Hospital in China were included (Figure 2). Eighty-six cases were excluded because of inadequate samples or unavailable biopsy results. Of the 644 eligible candidates, 479 (74.4%) patients received a specific diagnosis. Malignancy accounted for the etiology in most cases (262/644, 40.7%), followed by tuberculosis (217/644, 33.7%).

Figure 2 Results of closed pleural biopsy.

The demographic characteristics of patients with a specific diagnosis in both hospitals included age, sex, smoker or not, and the side and color of effusion. Protein, glucose, and ADA levels were also collected (Table 1). The average age of the patients was 54.7 years, and 305 males and 174 females were included.

Table 1 Patients’ demographic characteristics in Jinling and Jiangning hospital
Full table

As shown in Tables 2,3, the sensitivity of CPB in detecting MPE and TPE was 51.5% and 68.7%, respectively. The specificity and positive predictive value of CPB for MPE and TPE were both 100%, whereas the negative predictive value was 63.1% and 79.4% in MPE and TPE, respectively. The diagnostic yields of similar studies are also listed in Table 4.

Table 2 Closed pleural biopsy results, diagnosed as malignancy*
Full table

Table 3 Closed pleural biopsy results, diagnosed as tuberculosis
Full table

Table 4 Diagnostic yield of CPB in similar studies
Full table

The etiological classification for MPE is set out in Table 5. The most frequent histopathological type of MPE was pleural metastasis of pulmonary adenocarcinoma (204/262), followed by pulmonary squamous cell carcinoma (11/262), and small cell lung cancer (11/262). Lymphoma and mesothelioma accounted for 3.4% (9/262) and 2.3% (6/262) of MPEs, respectively. Other histopathological types are also listed in Table 5.

Table 5 Etiological diagnosis for malignant pleural fluid in Jinling and Jiangning Hospital
Full table

Table 6 shows the pleural fluid parameters of both the TPE group and the MPE group. There were significant differences in ADA, protein, and glucose between the groups. The mean values of ADA and protein in the TPE group were 48.83 U/L and 50.12 g/L, respectively, which were higher than the ADA and protein levels in the MPE group (15.09 U/L and 45.38 g/L, respectively). However, the MPE group had higher glucose levels (6.13 mmol/L) compared to the TPE group (5 mmol/L). LDH was slightly higher in malignant diseases than tuberculous lesions, although there were no significant differences.

Table 6 Pleural fluid parameters in TPE group and MPE group
Full table

Discussion

Since 1955, CPB has become a popular technique for diagnosing exudative pleural effusion (4). We performed a double-center retrospective analysis of the diagnostic yield of CPB in patients with exudative pleural fluid. The sensitivity of CPB for diagnosing TPE was significantly higher than for diagnosing MPE in our study. The relatively lower yield for MPE is due to the scarce, irregular, and patchy distribution of tumor invasion of the pleura, which can be improved by locating the focus through ultrasound or CT. The sensitivity for diagnosing MPE by CPB in our study was lower than that reported in some previous studies (11,14,18,19) but higher than that published by other teams (6,15,20,21). The diagnostic sensitivity of CPB in MPE ranged from 33.9% to 82.4%, which might be related to the technical level of operation or number of biopsies, for example. The diagnostic yield of CPB for TPE ranges from 60% to 95% according to previous reports (19,22-25). In our study, the sensitivity for TPE was 68.7%, which is consistent with previous studies.

While the specificity of CPB achieved 100% in both tuberculous and malignant pleural fluid, which is comparable with previous results (6,11,14,19,21), the positive predictive value was 100% in both TPE and MPE in our study, while the negative predictive value was lower (63.1% and 79.4% in the MPE and TPE groups, respectively). The reasons for MPE varied. Lung adenocarcinoma was the most frequent etiology, accounting for 77.7%, followed by pulmonary squamous carcinoma and small cell lung cancer, which each accounted for 4.1% of MPE cases. Mesothelioma and tumors of other systems, such as thymoma, lymphoma, metastatic carcinoma, made up the remaining etiologies.

As shown in Table 6, the ADA of pleural fluid in the TPE group was significantly higher than that in the MPE group, which demonstrated ADA to be an excellent parameter for distinguishing tuberculous from MPE. The sensitivity of ADA in the diagnosis of TPE in our study was 76.9%, slightly lower than the 91.9% sensitivity reported by Darooei et al. (26). The protein level in the TPE group was significantly higher than that in the MPE group, which is consistent with Valdés et al.’ findings but opposite to Darooei et al.’s (26,27). Antonangelo et al. also reported higher protein concentration in patients with TPE compared with MPE (P<0.001) (28). In contrast, the glucose level was lower in the TBE group (mean: 5 mmol/L) compared to the MPE group (mean: 6.13 mmol/L). This did not correspond to the findings of a previous report by Darooei et al. and Herrera et al. (26,29).

This is double-center retrospective research with large samples, involving 479 patients who were specifically diagnosed. We demonstrated that the sensitivity of CPB for MPE and TPE was 51.5% and 68.7%, respectively. The results showed that CPB had a higher sensitivity in diagnosing TPE, whereas the diagnostic yield for MPE was relatively low. The main reason for this relatively low diagnostic yield was the non-uniform pleural involvement of primary diseases, which caused the failure of obtaining the focus through biopsy needle. More evidence showed that medical thoracoscopy and video-assisted thoracoscopic surgery played important roles in diagnosing pleural diseases with high sensitivity (9,30-33).

However, medical thoracoscopy and video-assisted thoracoscopic surgery are more invasive and expensive than CPB, and they are difficult to carry out in primary hospitals. Image-guided pleural biopsy is not popular, especially in primary hospitals, because it requires more equipment and a higher level of training for physicians. CPB is still widely performed in patients with undiagnosed pleural effusion at our institution for its advantages of simple manipulation, minimal trauma, minimal pain, low cost, and safety. It is still a valuable diagnostic procedure and should be performed for patients with undiagnosed pleural effusion in clinical practice.

Our study’s most notable limitation was its retrospective nature. Furthermore, we excluded non-specific diagnoses, which might be malignancy or tuberculous, because we did not follow up with these patients to make a firm diagnosis. Another potential limitation is the inequality in the technical ability of different physicians. Nevertheless, the research included two centers and had a good sample size, which contributes to the quality of the study.

Conclusions

CPB has a higher sensitivity in the diagnosis of exudative pleural effusion, especially for tuberculous pleural diseases. For malignant pleural fluid, CPB showed a moderate diagnostic efficacy of over 50%. CPB could be a valuable technique in clinical practice, especially for basic-level hospitals.

Acknowledgments

Funding: This work was supported by grants from the National Natural Science Foundation of China (grant number 81401903, 81572937 and 81572273); the16^th batch “Summit of the Six Top Talents” Program of Jiangsu Province (grant number WSN-154); China Postdoctoral Science Foundation 12^th batch Special fund (Postdoctoral number: 45786);China Postdoctoral Science Foundation 64^th batch (Postdoctoral number: 45786); Jiangsu Provincial Postdoctoral Science Foundation (grant number 2018K049A); the Natural Science Foundation of Jiangsu province (grant number BK20180139 and BK20161386); Jiangsu Provincial Medical Youth Talent (grant number QNRC2016125), and the Nanjing Medical Science and Technology Development Project (No. ZKX17044), the Jiangsu Provincial Key Research and Development Program (No. BE2016721).

Footnote

Conflicts of Interest: All authors have completed the ICMJE uniform (available at http://dx.doi.org/10.21037/atm.2020.03.47). The authors have no conflicts of interest to declare.

Ethical Statement: The authors are accountable for all aspects of the work in ensuring that questions related to the accuracy or integrity of any part of the work are appropriately investigated and resolved. The study protocol was approved by the Ethical Committee of the Affiliated Jinling Hospital of Nanjing University and the Affiliated Jiangning Hospital of Nanjing Medical University (DBNJ027). Written informed consent was obtained from all patients.

Open Access Statement: This is an Open Access article distributed in accordance with the Creative Commons Attribution-NonCommercial-NoDerivs 4.0 International License (CC BY-NC-ND 4.0), which permits the non-commercial replication and distribution of the article with the strict proviso that no changes or edits are made and the original work is properly cited (including links to both the formal publication through the relevant DOI and the license). See: https://creativecommons.org/licenses/by-nc-nd/4.0/.

References

1. Fisk M, Branley H. Pleural effusion. Br J Hosp Med (Lond) 2013;74:C50-4. [Crossref] [PubMed]
2. Hooper C, Lee YC, Maskell N. Investigation of a unilateral pleural effusion in adults: British Thoracic Society Pleural Disease Guideline 2010. Thorax 2010;65 Suppl 2:ii4-17. [Crossref] [PubMed]
3. Defrancis N, Klosk E, Albano E. Needle biopsy of the parietal pleura. N Engl J Med 1955;252:948-51. [Crossref] [PubMed]
4. Cope C. New pleural biopsy needle; preliminary study. J Am Med Assoc 1958;167:1107-8. [Crossref] [PubMed]
5. Abrams LD. A pleural-biopsy punch. Lancet 1958;1:30-1. [Crossref] [PubMed]
6. Chakrabarti B, Ryland I, Sheard J, et al. The role of Abrams percutaneous pleural biopsy in the investigation of exudative pleural effusions. Chest 2006;129:1549-55. [Crossref] [PubMed]
7. Son HS, Lee SH, Darlong LM, et al. Is There a Role for a Needle Thoracoscopic Pleural Biopsy under Local Anesthesia for Pleural Effusions? Korean J Thorac Cardiovasc Surg 2014;47:124-8. [Crossref] [PubMed]
8. Haridas N, Suraj KP, Rajagopal TP, et al. Medical Thoracoscopy vs Closed Pleural Biopsy in Pleural Effusions: A Randomized Controlled Study. J Clin Diagn Res 2014;8:MC01-4. [PubMed]
9. Maturu VN, Dhooria S, Bal A, et al. Role of medical thoracoscopy and closed-blind pleural biopsy in undiagnosed exudative pleural effusions: a single-center experience of 348 patients. J Bronchology Interv Pulmonol 2015;22:121-9. [Crossref] [PubMed]
10. Dixon G, de Fonseka D, Maskell N. Pleural controversies: image guided biopsy vs. thoracoscopy for undiagnosed pleural effusions? J Thorac Dis 2015;7:1041-51. [PubMed]
11. Zuberi FF, Zuberi BF, Ali SK, et al. Yield of closed pleural biopsy and cytology in exudative pleural effusion. Pak J Med Sci 2016;32:356-60. [PubMed]
12. James P, Gupta R, Christopher DJ, et al. Evaluation of the diagnostic yield and safety of closed pleural biopsy in the diagnosis of pleural effusion. Indian J Tuberc 2010;57:19-24. [PubMed]
13. Al-Shimemeri AA, Al-Ghadeer HM, Giridhar HR. Diagnostic yield of closed pleural biopsy in exudative pleural effusion. Saudi Med J 2003;24:282-6. [PubMed]
14. Báez-Saldaña R, Rumbo-Nava U, Escobar-Rojas A, et al. Accuracy of closed pleural biopsy in the diagnosis of malignant pleural effusion. J Bras Pneumol 2017;43:424-30. [Crossref] [PubMed]
15. Pereyra MF, San-Jose E, Ferreiro L, et al. Role of blind closed pleural biopsy in the managment of pleural exudates. Can Respir J 2013;20:362-6. [Crossref] [PubMed]
16. Jakubec P, Kolek V, Václavík A, et al. Closed pleural biopsy in the diagnostics of malignant pleural involvement. Vnitr Lek 2014;60:423-30. [PubMed]
17. Botana-Rial M, Leiro-Fernández V, Represas-Represas C, et al. Thoracic ultrasound-assisted selection for pleural biopsy with Abrams needle. Respir Care 2013;58:1949-54. [Crossref] [PubMed]
18. Valdez-López HG, Cano-Rodríguez AI, Montemayor-Chapa M, et al. Diagnostic rentability of close pleural biopsy: Tru-cut vs. Cope. Rev Med Inst Mex Seguro Soc 2018;56:12-7. [PubMed]
19. Koegelenberg CF, Irusen EM, von Groote-Bidlingmaier F, et al. The utility of ultrasound-guided thoracentesis and pleural biopsy in undiagnosed pleural exudates. Thorax 2015;70:995-7. [Crossref] [PubMed]
20. Mishra AK, Verma SK, Kant S, et al. A study to compare the diagnostic efficacy of closed pleural biopsy with that of the thoracoscopic guided pleural biopsy in patients of pleural effusion. South Asian J Cancer 2016;5:27-8. [Crossref] [PubMed]
21. Maskell NA, Gleeson FV, Davies RJ. Standard pleural biopsy versus CT-guided cutting-needle biopsy for diagnosis of malignant disease in pleural effusions: a randomised controlled trial. Lancet 2003;361:1326-30. [Crossref] [PubMed]
22. Sahn SA. State of the art. The pleura. Am Rev Respir Dis 1988;138:184-234. [Crossref] [PubMed]
23. Avnon L, Kalchiem-Dekel O, Gozlan-Talmor A, et al. The role of closed pleural biopsy in the diagnosis of tuberculous pleurisy in a population at-risk. Harefua 2016;155:110-4, 130-1.
24. Mestitz P, Purves MJ, Pollard AC. Pleural biopsy in the diagnosis of pleural effusion; a report of 200 cases. Lancet 1958;2:1349-53. [Crossref] [PubMed]
25. Bibby AC, Maskell NA. Pleural biopsies in undiagnosed pleural effusions; Abrams vs image-guided vs thoracoscopic biopsies. Curr Opin Pulm Med 2016;22:392-8. [Crossref] [PubMed]
26. Darooei R, Sanadgol G, Gh-Nataj A, et al. Discriminating Tuberculous Pleural Effusion from Malignant Pleural Effusion Based on Routine Pleural Fluid Biomarkers, Using Mathematical Methods Tanaffos 2017;16:157-65. [J]. [PubMed]
27. Valdés L, San-José E, Ferreiro L, et al. Predicting malignant and tuberculous pleural effusions through demographics and pleural fluid analysis of patients. Clin Respir J 2015;9:203-13. [Crossref] [PubMed]
28. Antonangelo L, Vargas FS, Seiscento M, et al. Clinical and laboratory parameters in the differential diagnosis of pleural effusion secondary to tuberculosis or cancer. Clinics 2007;62:585-90. [Crossref] [PubMed]
29. Herrera Lara S, Fernández-Fabrellas E, Juan Samper G, et al. Predicting Malignant and Paramalignant Pleural Effusions by Combining Clinical, Radiological and Pleural Fluid Analytical Parameters. Lung 2017;195:653-60. [Crossref] [PubMed]
30. Dole SS, Godbole GP, Pophale HS. To Study Efficacy of Medical Thoracoscopy in Undiagnosed Pleural Effusions. J Assoc Physicians India 2016;64:20-3. [PubMed]
31. McDonald CM, Pierre C, de Perrot M, et al. Efficacy and Cost of Awake Thoracoscopy and Video-Assisted Thoracoscopic Surgery in the Undiagnosed Pleural Effusion. Ann Thorac Surg 2018;106:361-7. [Crossref] [PubMed]
32. Thomas M, Ibrahim WH, Raza T, et al. Medical thoracoscopy for exudative pleural effusion: an eight-year experience from a country with a young population. BMC Pulm Med 2017;17:151. [Crossref] [PubMed]
33. Valsecchi A, Arondi S, Marchetti G. Medical thoracoscopy: analysis on diagnostic yield through 30 years of experience. Ann Thorac Med 2016;11:177-82. [Crossref] [PubMed]