Silver nitrate versus tetracycline in pleurodesis for malignant pleural effusions; a prospective randomized trial
Seyed Abass Tabatabaei, Seyed Mozafar Hashemi, Ali Kamali
Department of Thorax Surgery, Isfahan University of Medical Sciences, Isfahan, Iran
Date of Submission | 14-Jul-2013 |
Date of Acceptance | 15-Sep-2013 |
Date of Web Publication | 31-Aug-2015 |
Correspondence Address: Seyed Abass Tabatabaei Resident of Obstetrics and Gynecology, School of Medicine, Isfahan University of Medical Sciences, Isfahan Iran
 Source of Support: Nil, Conflict of Interest: None declared.  | Check |
DOI: 10.4103/2277-9175.164007
Background: In this study, we aimed to investigate the effectiveness of silver nitrate (SN) versus tetracycline in pleurodesis among patients with malignant pleural effusion (MPE). Methods: In this prospective randomized clinical trial, patients with unilateral MPE candidate for pleurodesis were enrolled. The patients randomly allocated in two groups for receiving 20 mL 0.5% SN or 2.5 g tetracycline diluted in 30 cc normal saline and 0.1% lidocaine, through the chest tube. Patients were followed-up immediately (during 24 h) and 1-month after the procedure for evaluating recurrence of the pleural effusion using chest radiograph. They were clinically evaluated for chest pain and/or dyspnea and fever using a questionnaire that completed by the surgeon. The results were compared with two groups. Results: During this trial, 50 patients with MPE candidate for pleurodesis were selected and randomized into two interventional groups (25 patients in each group). Immediate and late recurrence of pleural effusion after pleurodesis were similar in two groups (P > 0.05). All patients in tetracycline group had fever and chest pain, but in SN group fever and chest pain were reported in 3 (12%) and 12 (48%) of patients, respectively (P < 0.05). Conclusion: SN is at least as effective as tetracycline for MPE treatment. In addition, its side effects were lower than tetracycline. Other advantages of SN are its low cost, availability, and safety. For more accurate results, it is recommended to design further trials with larger sample size and with lower doses of both SN and tetracycline. Keywords: Malignant plural effusion, pleurodesis, silver nitrate, tetracycline
How to cite this article: Tabatabaei SA, Hashemi SM, Kamali A. Silver nitrate versus tetracycline in pleurodesis for malignant pleural effusions; a prospective randomized trial. Adv Biomed Res 2015;4:178 |
How to cite this URL: Tabatabaei SA, Hashemi SM, Kamali A. Silver nitrate versus tetracycline in pleurodesis for malignant pleural effusions; a prospective randomized trial. Adv Biomed Res [serial online] 2015 [cited 2023 May 30];4:178. Available from: https://www.advbiores.net/text.asp?2015/4/1/178/164007 |
Introduction | |  |
Malignant pleural effusion (MPE) is considered as one of the most important complications of malignancies that is related to the high rate of morbidity.[1] In addition, almost all patients will experience debilitating dyspnea that consequently reduce the quality of life of the affected patients.[2]
Currently available treatment for the management of MPE are pleurodesis, tunneled pleural catheters or repeated thoracentesis.[3],[4],[5] From which pleurodesis with chemical agents is the most commonly used technique.[3]
Pleurodesis is the obliteration of the pleural space by fusion of the visceral and parietal pleurae with fibrous tissue.[6] It is suggested that chemical agents used for the procedure, locally activates the coagulation system and production of fibrogenic cytokines and consequently production of collagen.[6]
It is well-established that an appropriate pleural sclerosing agent should be safe, widely available, inexpensive and easy to apply and should not cause significant side effects. However, the ideal agent has not identified yet, and there is not an agent meet all of the mentioned criteria.[7] Different agents including talc, antimalarials (quinacrine, mepacrine), antineoplastic (bleomycin, 5-fluorouracil, mitomicin, etc.), antibiotics (tetracyclines, minocycline, doxycycline), silver nitrate (SN), immunomodulating and biological agents have been investigated and different results have been achieved.[6],[8],[9],[10] It seems that the ideal pleural sclerosing agent for each setting should be selected according to the characteristics of the patients and facilities of the center.
Silver nitrate and tetracycline are the most commonly used chemicals for pleurodesis. Several studies have evaluated their effectiveness and side effects separately or in comparisons with each other's and various results have been reported.[11],[12],[13],[14] They are also the most frequently used agents in our surgical departments but since now no study have compared their effectiveness in the treatment of MPE.
So, considering the paramount importance of quality of life in patients with MPE and selection of appropriate technique with low complication and sufficient efficacy for treatment of this group of patients, we aimed to investigate whether these chemicals could perform efficient and safe pleurodesis with less side effects and which of them is superior.
Methods | |  |
In this prospective randomized clinical trial patients with unilateral MPE candidate for pleurodesis and admitted to the surgery Department of Alzahra Hospital affiliated to the Isfahan University of Medical Sciences were enrolled.
Patients with MPE who has the following criteria were included in the study:
- Anticipated survival longer than 1-month
- Having dyspnea or improved respiratory symptoms due to the effusion
- Cytologicaly or histologically confirmed MPE.
Patients with MPE who had following characteristics were excluded from the study:
- Inappropriate expansion of lungs during drainage of the effusion by tube thoracostomy
- Pulmonary involvement with tumoral mass
- Patients with air leak or history of previous pleurodesis
- History of any interpleural therapy or radiation therapy on the affected hemithorax.
The protocol of the study was approved by the regional ethics committee of Isfahan University of Medical Sciences. Written informed consent was obtained from all selected patients.
In all selected patients, a chest tube (26 For 28 F) was placed using local anesthesia. Plural effusion was drinaged and the patients were prepared for pleurodesis. The patients randomly allocated in two groups for receiving 20 mL 0.5% SN (Merck; Darmstadt, Germany). Or 2.5 g tetracycline (Hakim Pharmaceutical Company-capsule 25 mg) diluted in 30 cc normal saline and 0.1% lidocaine, through the chest tube.
The sclerosant was injected to the patients in each group. The patients were placed in right and left decubitus, prone and supine positions for 10–15 min. The chest tube was unclamped after 1 h and removed when the amount of drinaged fluid reached to <100 cc. After removal of the chest tube, chest radiograph was performed for confirmation of the appropriate lung reexpantion. The patients were clinically evaluated for chest pain and/or dyspnea and fever using a questionnaire that completed by the surgeon.
Chest pain was recorded using a linear scale of 1–3 (1: Mild, 2: Moderate and 3: Sever). Patients were said to have dyspnea or chest discomfort if they have the symptoms more severe than that experienced before the procedure.
Patients were said to have fever if they had oral temperature >37.5°C.
Patients were followed-up immediately (during 24 h) and 1-month after the procedure for evaluating recurrence of the pleural effusion using chest radiograph. Characteristics of the patients were recorded, using a questionnaire. The data in two studied groups were compared.
Statistical analysis
Data analyzed using SPSS version 18 (SPSS Inc., Chicago, IL, U.S.A.) software. Qualitative variables were presented as number (%) and compared in studied groups using Chi-square test. Quantitive variables were presented as the mean ± standard deviation. The comparison of quantitative and qualitative variables between studied groups was done using one t-test and Chi-square test, respectively.
Results | |  |
During this trial, 50 patients with MPE candidate for plurodesis were selected and randomized in two interventional groups (25 patients in each group). The consort diagram of the study is presented in [Figure 1].
Characteristics of the patients allocated in two interventional groups are presented in [Table 1]. | Table 1: Characteristics of the patients with malignant plural effusion allocated to received silver nitrate and tetracycline
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Frequency of recurrence rate of plural effusion and complications of pleurodesis including fever, pain and dyspnea and/or chest discomfort in two studied groups are presented in [Figure 2]. | Figure 2: Frequency of recurrence rate of plural effusion and complications of plurodesis including fever, chest pain and/or dyspnea in patients with malignant plural effusion allocated to received silver nitrate and tetracycline
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Chest pain after pleurodesis was severed and moderate in 16 (64%) and 9 (36%) of patients in tetracycline group, respectively.
Moderate and mild chest pain after pleurodesis were reported in 1 (4%) and 11 (44%) of patients in SN group, respectively.
Discussion | |  |
In this trial, we have investigated both effectiveness and complications of SN versus tetracycline in pleurodesis for MPE. The results indicated that effectiveness of the two agents was similar but regarding the complications, SN was a more appropriate agent.
As mentioned, there is much debate regarding selection of the most appropriate chemical agent for pleurodesis. According to the report of a review study, the most effective agents are oral forms of tetracycline derivatives, quinacrine, SN, iodopovidone, and talc.[15],[16]
Though many novel agents such as doxcycline have been introduced also,[17] but we studied the effectiveness of agents which most commonly used in our settings. However, Shouman et al. have indicated that the most important factors for choosing a sclerosing agent in developing countries are the drug availability and cost.[18]
In this study, breast and lung cancer were the most common types of malignancies that result in MPE in both studied groups. It was in line with other studies. Previous studies indicated that about 75% of MPE are secondary to the lungs, breast cancers or lymphoma.[19] In another study in 50–65% of cases of MPE, lung and breast cancer were the most frequent causes.[20]
The success rate of pleurodesis in SN and tetracycline groups were 76% and 84%, respectively. Though our results were similar to the rates have been reported in previous studies,[21],[22],[23] but comparing the effectiveness of studied agents with other studies is so difficult due to the fact that different doses of the agents and various techniques for pleurodesis including tube size, differences in tube thoracostomy procedure and various definitions for success rate was applied.[20],[21]
Success rate of the two studied agents was similar in the current study.
There were few studies that compare these two therapeutic agents. Most of them were experimental and compared the agents with others. In addition, there was not any clinical trial for comparing the two agents. The First experimental study that compared the effectiveness of SN versus tetracycline was carried out in rabbits by Vargas et al. in Brazil. They showed that intrapleural injection of 0.50% SN produced an effective pleurodesis as well as 35 mg/kg tetracycline with no significant side effects. They concluded that SN is comparable to tetracycline.[22]
There were many studies regarding the effectiveness of SN and tetracycline.[11],[12],[13],[14]
Evidences indicated that tetracycline stimulates mesothelial cell release of growth factors for fibroblast proliferation and deposition of collagen. It is dose-dependent effective inhibitors of the matrix-degrading metalloproteinase (MMP) activity in the pleural fluid. Therefore, it reduces the activity of MMPs and remodels the tissues by normal repairs not fibrosis.[23]
The doses of tetracycline that used in current study was higher than prior studies (2.5 g vs. 0.5–1.5 g in other studies),[11],[24] whereas the success rate of studies which used lower doses of tetracycline were similar to ours, so it is recommended to study different doses of tetracycline for pleurodesis in patients with MPE.
The effectiveness of SN for pleurodesis is due to its induced caustic injury to the mesothelium, and its effectiveness has been proven in many experimental and few clinical studies.[±11],[25],[26] According to that studies SN 0.5% could be an appropriate alternative to tetracycline with low adverse effects.[22] In addition, recent studies have demonstrated the effectiveness of low dose SN that is, 0.1% for pleurodesis.[27] It could be also used used in some conditions such as an early bronchopleural fistula.[28] In our study, SN had similar success rate to tetracycline and lower side effect. Its priority to tetracycline was its lower adverse effects. Considering that a lower dose of SN (0.1) could have a similar effect and obviously lower adverse consequences, so further studies for evaluating different doses of SN would be more practical.
The main limitation of our study was the small sample size of patients.
The strength of the current study was its design. Because most of the previous studies were experimental and in animals, and there were few clinical trials in this field.
Conclusion | |  |
The findings of the current study showed that SN is at least as effective as tetracycline. In addition, its side effects were lower than tetracycline. Other advantages of SN are its low cost, availability and safety. For more accurate results, it is recommended to design further trials with larger sample size and with lower doses of both SN and tetracycline.
In addition, it seems that comparing the effectiveness and complications of other low-cost agents with SN would be more helpful to obtain more accurate and practical results in this field.
References | |  |
1. | Uzbeck MH, Almeida FA, Sarkiss MG, Morice RC, Jimenez CA, Eapen GA, et al.Management of malignant pleural effusions. Adv Ther 2010;27:334-47. |
2. | Arber A, Clackson C, Dargan S. Malignant pleural effusion in the palliative care setting. Int J Palliat Nurs 2013;19:320, 2-5. |
3. | Suárez PM, Gilart JL. Pleurodesis in the treatment of pneumothorax and pleural effusion. Monaldi Arch Chest Dis 2013;79:81-6. |
4. | Muduly D, Deo S, Subi TS, Kallianpur A, Shukla N. An update in the management of malignant pleural effusion. Indian J Palliat Care 2011;17:98-103.  [ PUBMED] |
5. | Nam HS. Malignant pleural effusion: Medical approaches for diagnosis and management. Tuberc Respir Dis (Seoul) 2014;76:211-7. |
6. | Bakr RM, El-Mahalawy II, Abdel-Aal GA, Mabrouk AA, Ali AA. Pleurodesis using different agents in malignant pleural effusion. Egypt J Chest Dis Tuberc 2012;61:399-404. |
7. | Lee YC, Baumann MH, Maskell NA, Waterer GW, Eaton TE, Davies RJ, et al.Pleurodesis practice for malignant pleural effusions in five English-speaking countries: Survey of pulmonologists. Chest 2003;124:2229-38. |
8. | Hashemzadeh S, Hashemzadeh K, Mamaghani K, Ansari E, Aligholipour R, Golzari SE, et al.Pleurodesis by erythromycin, tetracycline, Aerosil™ 200, and erythromycin plus Aerosil™ 200 in a rat model: A preliminary study. Daru 2012;20:79. |
9. | Dikensoy O, Light RW. Alternative widely available, inexpensive agents for pleurodesis. Curr Opin Pulm Med 2005;11:340-4. |
10. | Bouros D, Froudarakis M, Siafakas NM. Pleurodesis: Everything flows. Chest 2000;118:577-9. |
11. | Tremblay A, Stather DR, Kelly MM. Effect of repeated administration of low-dose silver nitrate for pleurodesis in a rabbit model. Respirology 2011;16:1070-5. |
12. | Terra RM, Kim SY, Pego-Fernandes PM, Teixeira LR, Vargas FS, Jatene FB. Is silver nitrate pleurodesis for patients with malignant pleural effusion feasible and safe when performed in an outpatient setting? Ann Surg Oncol 2011;18:1145-50. |
13. | Krasnik M, Christensen B, Halkier E, Høier-Madsen K, Jelnes R, Wied U. Pleurodesis in spontaneous pneumothorax by means of tetracycline. Follow-up evaluation of a method. Scand J Thorac Cardiovasc Surg 1987;21:181-2. |
14. | Tettey M, Sereboe L, Edwin F, Frimpong-Boateng K. tetracycline pleurodesis for malignant pleural effusion – A review of 38 cases. Ghana Med J 2005;39:128-31. |
15. | Chen H, Brahmer J. Management of malignant pleural effusion. Curr Oncol Rep 2008;10:287-93. |
16. | Mohamed KH, Hassan OA. A new look at an old agent for pleurodesis. Egypt J Chest Dis Tuberc 2013;62:617-20. |
17. | Rafiei R, Yazdani B, Ranjbar SM, Torabi Z, Asgary S, Najafi S, et al.Long-term results of pleurodesis in malignant pleural effusions: Doxycycline vs Bleomycin. Adv Biomed Res 2014;3:149. |
18. | Shouman W, Elgazzar A, Hussien RM, El Shaaray M, Light RW. Chemical pleurodesis for malignant pleural effusion. Egypt J Chest Dis Tuberc 2012;61:115-20. |
19. | Musani AI. Treatment options for malignant pleural effusion. Curr Opin Pulm Med 2009;15:380-7. |
20. | Light RW, Lee YC. Textbook of Pleural Diseases. Ch. 22. London: Arnold Publisher; 2003. p. 97. |
21. | Kilic D, Akay H, Kavukçu S, Kutlay H, Cangir AK, Enön S, et al.Management of recurrent malignant pleural effusion with chemical pleurodesis. Surg Today 2005;35:634-8. |
22. | Vargas FS, Teixeira LR, Silva LM, Carmo AO, Light RW. Comparison of silver nitrate and tetracycline as pleural sclerosing agents in rabbits. Chest 1995;108:1080-3. |
23. | Marshall BC, Santana A, Xu QP, Petersen MJ, Campbell EJ, Hoidal JR, et al.Metalloproteinases and tissue inhibitor of metalloproteinases in mesothelial cells. Cellular differentiation influences expression. J Clin Invest 1993;91:1792-9. |
24. | Wallach HW. Intrapleural tetracycline for malignant pleural effusions. Chest 1975;68:510-2. |
25. | Menna C, Andreetti C, Ibrahim M, Maurizi G, Poggi C, Barile R, et al.The effect of silver nitrate pleurodesis after a failed thoracoscopic talc poudrage. Biomed Res Int 2013;2013:295890. |
26. | Paschoalini Mda S, Vargas FS, Marchi E, Pereira JR, Jatene FB, Antonangelo L, et al.Prospective randomized trial of silver nitrate vs talc slurry in pleurodesis for symptomatic malignant pleural effusions. Chest 2005;128:684-9. |
27. | Marchi E, Vargas FS, Acencio MM, Antonangelo L, Teixeira LR, Light RW. Low doses of silver nitrate induce pleurodesis with a limited systemic response. Respirology 2009;14:885-9. |
28. | Andreetti C, D'Andrilli A, Ibrahim M, Poggi C, Maurizi G, Vecchione A, et al.Submucosal injection of the silver-human albumin complex for the treatment of bronchopleural fistula. Eur J Cardiothorac Surg 2010;37:40-3. |
[Figure 1], [Figure 2]
[Table 1]
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