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Usual Interstitial Pneumonia with Lung Cancer: Clinicopathological Analysis of 43 Cases
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Original Article
Usual Interstitial Pneumonia with Lung Cancer: Clinicopathological Analysis of 43 Cases
Dae Hyun Song, In Ho Choi, Sang Yun Ha, Kang Min Han, Jae Jun Lee, Min Eui Hong, Kyeongman Jeon1, Man Pyo Chung1, Jhingook Kim2, Joungho Han
Korean Journal of Pathology 2014;48(1):10-16.
DOI: https://doi.org/10.4132/KoreanJPathol.2014.48.1.10
Published online: February 25, 2014

Department of Pathology, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea.

1Department of Internal Medicine, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea.

2Department of Thoracic Surgery, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea.

Corresponding Author: Joungho Han, M.D. Department of Pathology, Samsung Medical Center, Sungkyunkwan University School of Medicine, 81 Irwon-ro, Gangnam-gu, Seoul 135-710, Korea. Tel: +82-2-3410-2800, Fax: +82-2-3410-0025, 'hanjho@skku.edu'
• Received: October 23, 2013   • Revised: January 8, 2014   • Accepted: January 20, 2014

© 2014 The Korean Society of Pathologists/The Korean Society for Cytopathology

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0/) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

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  • Background
    Previous studies have suggested an association between usual interstitial pneumonia (UIP) and lung cancer (Ca). However, clinical and histological information is not enough to determine such an association, due to the low incidence and short survival time of patients with both conditions.
  • Methods
    We retrospectively reviewed the clinical and histological records of Ca patients with UIP between January 1999 and August 2013 at the Samsung Medical Center, Seoul, Korea. We found 43 patients who had Ca with UIP (UIP-Ca). Previously reported data of eighty-four patients with UIP-only were included as a comparison group.
  • Results
    Smoking is related to poor prognosis in patients with UIP-Ca, and the number of patients with a high smoking index of more than 30 pack-years significantly increased in UIP-Ca patients compared with UIP-only patients. There is no significant prognostic differentiation between UIP-Ca patients and UIP-only patients. Microscopically, UIP-Ca patients showed characteristically heterogeneous histological patterns and degrees of differentiation. There were many foci of squamous metaplasia or dysplasia at the peripheral area of squamous cell carcinomas.
  • Conclusions
    We report 43 cases of UIP-Ca. Our results suggest that smoking is related to cancer occurrence in UIP patients and poor prognosis in UIP-Ca patients.
Idiopathic interstitial pneumonia is classified into four categories: usual interstitial pneumonia (UIP), desquamative interstitial pneumonia, nonspecific interstitial pneumonia, and acute interstitial pneumonia.1,2 UIP, which is clinically known as idiopathic pulmonary fibrosis (IPF), is notorious for its poor prognosis, with a median survival of 2.8 to 5 years.3,4 Some studies have suggested an association between UIP and lung cancer,4-6 but reliable clinical and histological information regarding lung neoplasms in patients with UIP is scarce due to the rarity of the simultaneous occurrence of these conditions. Herein, we discuss the clinicopathological characteristics and analyze the survival probability of lung cancer patients with UIP.
Case selection
We collected data from lung cancer patients with UIP between January 1999 and August 2013 from the Samsung Medical Center, Seoul, Korea. A total of 46 patients were detected. These patients showed clinically appropriate operability and resectability, and pneumonectomy, lobectomy, sleeve lobectomy or wedge resection was performed. Three patients with connective tissue disease, including one patient with systemic sclerosis, one patient with CREST syndrome, and one patient with Sjogren syndrome, which are known risk factors for interstitial lung disease, were excluded. The remaining 43 patients had no drug or occupational history. Preoperative computed tomographies were examined. Gross findings, hematoxylin and eosin and immunohistochemical slides of surgical specimens were reviewed by two pathologists. Simultaneous diagnosis of lung cancer and UIP was found in twenty of the 43 patients (47%) (Tables 1, 2). The remainder showed the diagnostic time of precedent UIP and subsequent lung cancer. The cancer-free period (CFP) is defined as the period of UIP before the detection of lung cancer (e.g., a CFP of zero means UIP and lung cancer were diagnosed at the same time).
Microscopically, all cases showed lung cancers at the background of UIP. The Institutional Review Board approved this study (SMC 2013-08-149-001).
Reference data as comparison group
Clinical data of eighty-four patients with UIP without lung cancer from a previous report was included for comparison (Table 3).7 These 84 patients were diagnosed at our hospital between July 1996 and June 2002. Fifty-seven of the 84 patients were histologically diagnosed by surgical lung biopsy and the remaining twenty-seven patients were identified by the nonhistological diagnostic criteria of the American Thoracic Society.8 Identical exclusion criteria were used for reference group selection.
Statistical analysis
The overall survival of patients with lung cancer and UIP and patients in the reference group was compared using the multivariate analysis of the Cox proportional hazard model. Correlation analysis was performed using chi-squared tests and independent t-tests. Values were considered statistically significant at a p-value less than .05. All statistical analyses were performed in SPSS ver. 12.0 (SPSS Inc., Chicago, IL, USA).
Of the 43 patients, 41 (95%) were male and 34 (79%) were smokers. The smokers included 14 current and 20 ex-smokers. The mean age was 68 years. Thirty-seven (86%) patients received a lobectomy, and 33 (77%) instances of lung cancer were located in the lower lobe. The lung cancers consisted of 18 squamous cell carcinomas, 17 adenocarcinomas, 2 combined carcinomas, 2 large cell neuroendocrine carcinomas, and a number of other less common neoplasms. The combined carcinomas consisted of squamous cell carcinoma with a large cell neuroendocrine carcinoma, and small cell carcinoma with a non-small cell carcinoma.
Compared to the reference data, older age and male sex were significantly associated with lung cancer in patients with UIP (Table 4). In addition, positive smoking history and more than 30 pack-years of smoking (mean cigarette number per day multiplied by smoking years) were higher in the UIP with lung cancer group than in the UIP-only group (Table 4).
Survival analysis results revealed a 1-year survival rate of 60% for patients with lung cancer and UIP. Multivariate analysis of the Cox proportional hazard model was performed with factors of age, stage, surgical procedure, smoking history, smoking index and pulmonary function test before surgery in the 43 UIP with lung cancer patients and in the total 127 patients, including the 84 UIP-only patients (Tables 5, 6). Except for smoking history, all factors showed no significant correlation with survival. In the 43 UIP with lung cancer patients, those with smoking history had an odds ratio of 12.610 (95% confidence interval [CI], 1.293 to 123.016; p=.029) relative to the nonsmoking patients. In the group of all 127 patients, the patients with smoking history had an odds ratio of 1.557 (95% CI, 0.799 to 3.033; p=.193) relative to the nonsmoking patients. In addition, an odds ratio of 0.461 was found between the UIP with cancer and the UIP-only patients.
The causes of death were examined. Metastasis of lung cancer occurred to the spine in one patient, to the pleura in one patient and to the lung in the other 5 patients. Thirteen patients died due to pulmonary failure with pneumonia. Acute respiratory distress syndrome and acute renal failure occurred in three patients with a survival period of less than 1 month. The remaining 23 patients were censored or had no clinical record.
Histopathologically, on gross examination, all tumors were located at the UIP lesion. Almost all tumors were poorly circumscribed and were 0.4 to 7.5 cm in size. The UIP lesion was found to be firm and poorly circumscribed in appearance with a honeycombing pattern. Microscopically, UIP was detected in the peritumoral area in all cases. The UIP showed nonuniform interstitial fibrosis with a patchwork pattern, fibroblastic foci, mild inflammation and honeycomb changes (Figs. 1, 2A). Several areas with hyperplasia of bronchial smooth muscle were detected. There were frequent areas of brown pigmented macrophages in the air spaces and interstitia.
Squamous cell carcinoma with UIP
Eighteen of the 43 lung cancers were squamous cell carcinomas. Twelve cases were moderately differentiated, 5 cases were poorly differentiated and 1 case was well differentiated. The patient with a well-differentiated squamous cell carcinoma (case no. 43) had a comparatively longer survival period. Microscopically, the structure of UIP was maintained in the tumoral areas, and cancer cell proliferation was observed along the cavernous hall of the honeycombing. The tumors showed variable degrees of differentiation. Wide dense fibrotic stroma was detected between the clusters of the squamous cell carcinomas. Peritumoral UIP lesions occasionally showed squamous metaplasia or dysplastic epithelial cells (Fig. 2). The foci of squamous metaplasia were haphazardly distributed along the cavernous hall of honeycombing.
Adenocarcinoma with UIP
Seventeen of the 43 lung cancers were adenocarcinomas. Microscopically, dense fibrotic stroma and large cavities of honeycombing were discovered in the tumoral areas. The adenocarcinomas also grew along the cavernous halls of honeycombing rather than invading the fibrotic stroma. The growth patterns varied at tumors and were described as acinar, papillary, micropapillary or solid with cavitation.9,10 The acinar pattern with branching was the most frequently observed (Fig. 2F), followed by papillary and micropapillary patterns (Fig. 2E). One case showed a mainly solid pattern. Most of the adenocarcinomas accompanied clear cell changes (Fig. 2G). Clear cells had distinct cell borders that had plump clear to pinkish cytoplasm and round nuclei with smooth and slightly thickened membranes. Several areas of intracellular or extracellular mucin production (Fig. 2H) were detected. In addition, there were many foci of transformation from normal bronchiolar epithelium to adenocarcinomas in the peripheral tumor areas (Fig. 2C, D).
UIP is a fatal interstitial fibrosing disease of the lung. In recent studies, a similarity between UIP and lung cancer has been suggested based on epigenetic and genetic abnormalities, pathogenetic sequence, a shared feature of uncontrolled proliferation and abnormalities of specific signaling pathways in UIP.11,12 UIP is also known to increase the risk of lung cancer.6 Although there are only a few reports regarding lung cancer in patients with UIP, they commonly describe a predominance of squamous cell carcinoma, male sex and a positive history of smoking.5 Our study also showed a significantly higher incidence in older or male patients compared to a reference group. UIP patients with lung cancer showed higher rates of smoking history (p=.113) and more than 30 pack-years of smoking (p=.052). According to several previous reports,5,6,13 smoking ought to be related to UIP with lung cancer. Our study also shows such a relationship. We also found many foci of squamous metaplasia at the periphery of squamous cell carcinomas. Considering the well-known relationship between smoking and squamous metaplasia, we suggest smoking as a pathogen of lung cancer in UIP patients. Calabrese et al.14 described the overexpression of squamous cell carcinoma antigens in IPF. They demonstrated that metaplastic epithelial cells play an important role in the tumorigenesis of UIP. There were many foci of squamous metaplasia in honeycombing epithelium in the present study. According to a report of Hironaka and Fukuyama,15 IPF patients with lung cancer showed more frequent foci of squamous metaplasia than IPF patients without lung cancer (p=.002). They suggested that squamous metaplasia may not be a precursor of lung cancer itself, but could cause a susceptibility to developing lung carcinoma on the basis of Ki67 and p53 indexes. As a result, smoking may promote tumorigenesis, and metaplastic and dysplastic foci of the UIP lesion suggest progression to lung cancer. We recommend that the amount of metaplastic or dysplastic foci be mentioned in the pathologic report of lung biopsies, and that UIP patients who have frequently metaplastic foci and more than 30 pack-years of smoking receive close follow-up.
Histologically, the major lung neoplasms identified in patients with UIP were squamous cell carcinoma and adenocarcinoma. These lesions showed a characteristically variable degree of differentiation and histological pattern. These disparate findings may be explained by two broad hypotheses regarding pathogenesis. 1) UIP background: UIP has heterogeneous microscopic features that lead to heterogeneous structural patterns and a variable degree of differentiation. 2) Synchronous dysplastic foci: many metaplastic and dysplastic foci were found in peritumoral UIP lesions. A neoplastic mass may be composed of several synchronous tumors originating from a single UIP lesion. This hypothesis of conjoined synchronous tumors can explain the variable degree of differentiation and structural patterns, as well as the incidence of combined tumors and tumors that are found soon after or at the same time patients are diagnosed with UIP.
In the survival analysis, the odds ratio between the cancer group and the no cancer group was 0.461. This indicates that there is no significant prognostic differentiation between the UIP with lung cancer group and the UIP-only group. Even though this study has a limitation of the previously reported comparison group, such a low value of the odds ratio has implications for clinical prognostic guidelines and Korean data.
In conclusion, we report a rare 43 cases of UIP with lung cancer. Smoking is related to poor prognosis in UIP patients with lung cancer, and the number of patients with high a smoking index of more than 30 pack-years significantly increased in UIP with lung cancer patients compared with UIP-only patients. There is no significant prognostic differentiation between UIP with lung cancer patients and UIP-only patients in multivariate analysis.

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

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Fig. 1
(A) Computed tomography horizontal view reveals a pulmonary mass with usual interstitial pneumonia (UIP). (B) The surgical specimen shows a poorly-circumscribed gray and white soft mass with UIP.
kjpathol-48-10-g001.jpg
Fig. 2
(A) On the low-power field, usual interstitial pneumonia (UIP) shows non-uniform interstitial fibrosis with a patchwork pattern, honeycomb changes, fibroblastic foci (inset) and mild inflammation (inset). (B) There are many dysplastic foci of the epithelium in the peripheral portion of this squamous cell carcinoma with UIP. (C) Adenocarcinomas also show many foci of transformation from normal bronchiolar epithelium to dysplastic cells at the periphery of the tumor. (D) Dysplastic cells show more hyperchromatic and larger nuclei than normal reactive bronchiolar epithelial cells. Adenocarcinomas have variable patterns described as micropapillary (E) and cleft-like acinar (F). (G) Most adenocarcinomas contain variable areas of clear cell change. (H) Several tumors show variable area of mucin production.
kjpathol-48-10-g002.jpg
Table 1.
Clinicohistological information of 43 usual interstitial pneumonia patients with lung cancer
Parameter n (%)
Sex (male) 41 (95)
Smoking history 34 (79)
Mean age (yr) 68
TNM stage
 I 19 (44)
 II 12 (28)
 III 11 (26)
 N/A 1 (2)
Surgical procedure
 Lobectomy 37 (86)
 Pneumonectomy 3 (7)
 Wedge resection 2 (5)
 Sleeve lobectomy 1 (2)
Histologic type
 Squamous cell carcinoma 18 (42)
 Adenocarcinoma 17 (40)
 LCNE 2 (5)
 Combined carcinoma 2 (5)
 Others 4 (9)
Location (lobe)
 Right lower 18 (42)
 Left lower 15 (35)
 Right upper 6 (14)
 Left upper 3 (7)
 Right middle 1 (2)
Less than 1 month of cancer-free period 20 (47)
1-Year survival rate 26 (60)

LCNE, large cell neuroendocrine carcinoma.

Table 2.
Clinicohistological information of 43 usual interstitial pneumonia patients with lung cancer
Case No. Age (yr) Sex Histologic type Size (cm) Lobe Segment T N M Stage Smoking SI (py) PFT FEV1/FVC (%) Procedure CFP (mo) SP (mo)
1 60 M SQ 3.5 LLL Superior 2a 1 0 IIA S N/A 89/81 P 0 0
2 70 M SQ 5.5 LLL Bronchus 2b 1 0 IIB E 35 108/101 S 58 0
3 66 M LCNE 2.5 RLL Posterior basal 1b 2 0 IIIA N 0 93/84 L 8 0
4 69 M SQ 7.5 LLL Basal 3 1 0 IIIA S N/A 65/84 L 0 1
5 71 M SQ 5 LUL Apicoposterior 2a 0 0 IB N 0 94/87 L 44 1
6 73 M SQ 6.8 LUL Anterior 2b 2 0 IIIA E 40 90/68 L 0 1
7 58 M Ad, SQ 2.8, 1.1 RUL Anterior 1b 0 0 IA E 25 77/85 L 60 1a
8 68 M Ad 4.5 LLL Posterior basal 2a 0 0 IB E 40 123/104 L 18 1
9 57 M Ad 2.2 LLL Anterior basal 2a 2 0 IIIA S 40 79/67 L 11 2
10 63 M SQ 4 RLL Lateral basal 2a 0 0 IB E 40 87/90 L 0 4a
11 59 M SQ 4.8 RLL Superior 2a 0 0 IB E 40 71/73 L 2 4a
12 72 M Ad 2 LLL Anterior basal 1a 0 0 IA N 0 110/89 L 2 4
13 67 M LCC 6 LLL Superior 2b 1 0 IIB S 60 93/90 P 0 6
14 75 M Ad 3.5 RLL Basal 2a 2 0 IIIA N 0 103/88 L 0 8
15 72 M LCNE 2.6 RLL Superior 2a 0 0 IB N 0 94/96 L 13 9
16 69 M LCNE+SQ 4 RML Bronchus 2a 2 0 IIIA E 30 107/110 L 48 10a
17 50 M Ad 3.5 LLL Posterior basal 2a 2 0 IIIA E N/A 75/70 L 48 10a
18 71 M SQ 1.8 RUL Anterior 1a 0 0 IA E 25 76/61 W 13 12a
19 73 M SQ 4.5 RLL Lateral basal 2a 2 0 IIIA E N/A 90/87 L 24 13a
20 66 M Ad 2.5 LLL Superior 2a 1 0 IIA E 44 108/94 L 20 13
21 74 M Ad 0.4 LLL Superior 1a 1 0 IIA S 60 118/105 L 1 15
22 71 M Ad 3 LLL Medial basal 3 2 0 IIIA S 49 80/89 L 20 15
23 76 M SQ 2.3 RUL Anterior 1b 0 0 IA E 50 83/77 L 0 16a
24 63 M SCC+NSCC 2.2 RUL Anterior N/A N/A N/A N/A S 20 88/77 W 1 17
25 70 M ASQ 4.5 RLL Lateral basal 1b 1 0 IIA E 47 96/82 L 84 17a
26 84 M Ad 1.7 RUL Posterior 1b 0 0 IA S 58 105/91 L 31 19
27 71 M Ad 4.8 RLL Lateral basal 2a 1 0 IIA S 45 122/113 L 0 20
28 76 M SQ 1.5 RLL Superior 1a 0 0 IA S 50 76/83 L 0 21
29 76 M Ad 2.2 LLL Superior 1b 2 0 IIIA S 20 100/91 L 0 22
30 79 M SQ × 2 1.9, 0.4 RLL Superior 2b 0 0 IIA E N/A 96/75 L 65 26a
31 65 M SQ 2 RLL Lateral basal 2a 0 0 IB E 38 90/85 L 0 29a
32 73 M SQ 3.1 LLL Posterior basal 2a 0 0 IB E 50 92/86 L 0 29a
33 70 M Pl 3.3 RLL Superior 2a 0 0 IB S N/A 104/85 L 0 30
34 70 M Ad 4.5 RLL Anterior basal 2a 0 0 IB N 0 124/107 L 0 33
35 68 M SQ 3 RLL Superior 4 2 0 IIIB N/A N/A 102/88 P 8 38
36 54 F Ad 3.5 RLL Anterior basal 2a 1 0 IIA N 0 82/75 L 0 40
37 63 M SQ 4 LLL Lateral basal 2a 0 0 IB S 60 96/77 L 17 43a
38 51 F Ad 2.5 RLL Superior 1b 0 0 IA N 0 87/71 L 0 53a
39 64 M Ad 1.8 RUL Anterior basal 2a 1 0 IIA E 40 123/99 L 6 56
40 73 M Ad 1 RLL Superior 1a 0 0 IA E N/A 79/81 L 0 63
41 71 M Ad 2.8 RLL Superior 1b 1 0 IIA S 60 95/103 L 0 82a
42 60 M SQ 3.5 LUL Anterior 2a 1 0 IIA E 40 106/97 L 0 117
43 67 M SQ 1.8 LLL Superior 2a 0 0 IB E 40 N/A L 0 160a

SI, smoking index; py, packyears; PFT, pre-operative pulmonary function test; FEV1, forced expiratory volume at 1 second; FVC, forced vital capacity; CFP, cancer-free period; SP, survival period; M, male; SQ, squamous cell carcinoma; LLL, left lower lobe; S, current smoker; N/A, not available; P, pneumonectomy; E, ex-smoker; LCNE, large cell neuroendocrine carcinoma; RLL, right lower lobe; N, non-smoker; L, lobectomy; LUL, left upper lobe; Ad, adenocarcinoma; RUL, right upper lobe; LCC, large cell carcinoma; LCNE+SQ, combined large cell neuroendocrine carcinoma and squamous cell carcinoma; RML, right middle lobe; W, wedge resection; SCC, small cell carcinoma; NSCC, non-small cell carcinoma; ASQ, adenosquamous carcinoma; Pl, pleomorphic carcinoma; F, female.

a Censored.

Table 3.
Clinical information of 84 usual interstitial pneumonia patients as a reference group
Parameter Value
No. of patients (surgical diagnosis:nonsurgical diagnosis) 57:27
Mean age (yr) 60
Sex (male:female) 66:18
Smoking history (N:E:C) 29:31:24
Mean survival period (mo)a 39.83 (2-117)

N, non-smoker; E, ex-smoker; C, current smoker.

a The dead:the censored=46:38.

Table 4.
Comparison between the UIP with lung cancer group and the UIP-only group
Lung cancer with UIP (n = 43) UIP-only (n = 84) p-value
Age (yr) 67.9 ± 7.2 60.3 ± 7.7 < .001
Sex (male:female) 41:2 (95.3) 65:19 (77.4) .01
Smoking history 34 (79.1) 55 (65.5) .113
More than 30 py 81.5% 60.0% .052

Values are presented as mean±standard deviation or number (%), unless indicated otherwise.

UIP, usual interstitial pneumonia; py, pack years.

Table 5.
Multivariate Cox proportional analysis of the 43 usual interstitial pneumonia with lung cancer patients
OR (95% CI) p-value
Smoking history (nonsmoking vs smoking) 12.610 (1.293-123.016) .029
Smoking index (≤ 30 py vs > 30 py) 0.528 (0.065-4.321) .552
FVC (> 86.5%a vs ≤ 86.5%) 0.342 (0.090-1.308) .117
Age (≤ 70a yr vs > 70 yr) 0.222 (0.070-0.709) .011
Stage (I vs II, III) 0.310 (0.100-0.957) .042
Procedure (W vs L, P) 0.026 (0.002-0.399) .009
CFP (≤ 2 mo vs > 2 mo) 0.188 (0.062-0.567) .003

OR, odds ratio; CI, confidence interval; Smoking, ex-smoker and current smoker; py, pack years; FVC, forced vital capacity; W, wedge resection; L, lobectomy; P, pneumonectomy; CFP, cancer free period.

a Median number.

Table 6.
Multivariate Cox proportional analysis of the total 127 patients, including the 43 UIP with lung cancer and 84 UIP-only patients
OR (95% CI) p-value
Smoking history (nonsmoking vs smoking) 1.557 (0.799-3.033) .193
Smoking index (≤ 30 py vs > 30 py) 0.913 (0.464-1.797) .792
FVC (≤ 80.5%a vs > 80.5%) 0.804 (0.480-1.347) .408
Age (≤ 63a yr vs > 63 yr) 0.699 (0.423-1.154) .161
Cancer (UIP-only vs UIP with cancer) 0.461 (0.262-0.810) .007

UIP, usual interstitial pneumonia; OR, odds ratio; CI, confidence interval; Smoking, ex-smoker and current smoker; py, pack years; FVC, forced vital capacity.

a Median number.

Figure & Data

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      Usual Interstitial Pneumonia with Lung Cancer: Clinicopathological Analysis of 43 Cases
      Korean J Pathol. 2014;48(1):10-16.   Published online February 25, 2014
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