Angiotensin II type 1 and 2 receptors and lymphatic vessels modulate lung remodeling and fibrosis in systemic sclerosis and idiopathic pulmonary fibrosis

Parra, Edwin Roger; Ruppert, Aline Domingos Pinto; Capelozzi, Vera Luiza

doi:10.6061/clinics/2014(01)07

Edwin Roger Parra

Faculdade de Medicina da Universidade de São Paulo, Department of Pathology, Laboratory of Histomorphometry and Pulmonary Genetics, São Paulo/SP, Brazil.

Aline Domingos Pinto Ruppert

Faculdade de Medicina da Universidade de São Paulo, Department of Pathology, Laboratory of Histomorphometry and Pulmonary Genetics, São Paulo/SP, Brazil.

Vera Luiza Capelozzi

Faculdade de Medicina da Universidade de São Paulo, Department of Pathology, Laboratory of Histomorphometry and Pulmonary Genetics, São Paulo/SP, Brazil.

All authors designed the study, analyzed and interpreted the data and wrote the manuscript.

No potential conflict of interest was reported.

E-mail: erparra20003@yahoo.com.br Tel.: 55 11 3066 7427

Figures (2)
Tables (3)

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Figure 1
Cellular expression of the angiotensin II type 1 receptor (AGTR-1) and AGTR-2 divided in septal areas and intrapulmonary vessels from normal control lungs, systemic sclerosis (SSc) and idiopathic pulmonary fibrosis (IPF). In (A) and (B), we observe a diffuse and minimal AGTR-1 (arrows) expression in the alveolar septal areas and in the intrapulmonary vessels of the controls. The AGTR-1 expression shows greater increases in the thickened alveolar septal region from the cellular SSc-NSIP (arrows, E) than in the fibrotic SSc-NSIP (arrows, I). In the intrapulmonary vessels, the expression of AGTR-1 (arrows) is minimal and similar in both groups (cellular SSc-NSIP, F and fibrotic SSc-NSIP, J). Increased expression of AGTR-1 (arrows) is observed in the septal areas (M) and intrapulmonary vessels (N) of IPF-UIP. In (C) and (D), we observed AGRT-2 (arrows) expression in the septal areas and intrapulmonary vessels from the controls. In (G) and (K), we observed a similar expression of AGTR-2 (arrows) in the septal areas of cellular and fibrotic SSc-NSIP. Increased expression of AGTR-2 (arrows) is observed in the intrapulmonary vessels of fibrotic SSc-NSIP (L) compared to cellular SSc-NSIP (H). The expression of AGTR-2 (arrows) is more evident in the septal areas of IPF-UIP (O) than in the intrapulmonary vessels (P) of this histologic pattern. Q and R show the total values of AGTR-1 and AGTR-2 and the results analyzed by a one-way ANOVA with the Bonferroni multiple comparisons test for the control, SSc-NSIP and IPF-UIP groups. (*) Significantly higher AGTR-1 expression was observed in the SSc-NSIP and IPF-UIP lungs compared with the control group (p = 0.001 and p = 0.001, respectively). A similar situation was observed with AGTR-2 expression from the SSc-NSIP and IPF-UIP patterns compared to the control group (p<0.001 and p<0.001, respectively). (†) Significantly higher expression of AGTR-2 in the SSc-NSIP group was observed when compared with the IPF-UIP group (p = 0.04) by Student's t-test.

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Figure 2
D2-40 cell expression in the lymphatic vessels of the normal control lungs, systemic sclerosis (SSc) and idiopathic pulmonary fibrosis (IPF). The lymphatic vessels (arrows) were observed in the sub pleural (A) and interlobular septal interstitium (B) in the control lungs. In cellular SSc-NSIP, the lymphatic vessels (arrows) were observed in the thickened alveolar septal region (C) and were infrequent compared to the fibrotic SSc-NSIP pattern (arrows, D). In the UIP pattern, we observed a higher proportion of lymphatic vessels (arrows) in the interlobular and subpleural spaces (E and F). G and H represent the total values of the lymphatic dilatation and density, and the results analyzed by the one-way ANOVA followed by the Bonferroni multiple comparisons test for the control, SSc-NSIP and IPF-UIP groups. (*) A significantly increased lymphatic dilatation (G) was observed in the IPF-UIP group compared to the SSc-NSIP (p = 0.01) and control (p = 0.01) groups. Similarly, a significantly higher lymphatic density (H) was observed in the IPF-UIP group compared to the SSc-NSIP (0.02) and control (0.01) groups.

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Table 1
Clinical data of the patients with systemic sclerosis and idiopathic pulmonary fibrosis.

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Table 2
Summary of the morphometric results^a. a The units of “% of points” indicate the number of points overlying the phenomena of interest divided by the total number of points overlying the septae and vessels. In morphometry, this process is called a point fraction and is often symbolized as Pp. The Pp has been shown to approximate the volume fraction or Vv.

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Table 3
Cox proportional hazards regression to ascertain the individual contribution of the histological patterns (NSIP and UIP) and the morphological factors associated with survival and to compare the adjusted survival between the groups (-2 log-likelihood = 59.93; Chi-squared = 40.10; p<0.001).

	SSc-NSIP (n = 30)	IPF-UIP (n = 26)	p-value
Age, years	45±8	64±7	<0.001
Sex (female/male)	30	10/16	1.2
Spirometry
FEV1 (% predicted)	70±13.8	76±20.01	0.23
FVC (% predicted)	65±13.8	69±16.8	0.35
FEV1/FVC	107±8.69	90±18.7	<0.001
TLC (% predicted)	81±11.5	78±21.9	0.64
RV (% predicted)	117±35.5	101±62.04	0.36
DLCO (% predicted)	66±21.6	55±19.1	0.01
DLCO/VA (% predicted)	77±35.2	47±22.74	0.008

Variables	Control	Cellular SSc-NSIP	Fibrotic SSc-NSIP	SSc-NSIP	UIP
Septal AGTR-1	1.45±1.02	10.72±6.20	12.18±8.00	11.41±6.97	10.10±22.23
Vascular AGTR-1	1.06±1.03	4.36±5.35	0.51±1.15	2.53±4.33	2.13±1.64
Septal AGTR-2	0.03±0.02	12.75±8.05	12.78±6.96	12.77±7.36	7.78±4.31
Vascular AGTR-2	0.01±0.04	1.26±1.35	6.91±4.64	3.83±4.30	6.06±4.66
Total AGTR-1	1.25±0.84	7.54±4.49	6.34±3.96	6.97±4.18	6.26±10.93
Total AGTR-2	0.02±0.02	6.51±3.88	9.85±5.09	8.18±4.73	6.38±3.63
Lymphatic density	1.68±0.38	2.72±0.62	2.92±0.69	2.80±0.65	3.73±1.19
Lymphatic area	2.81±0.90	4.28±1.32	4.33±0.64	4.25±1.08	5.52±2.24

	β	SE	Wald test	p-value	Exp (β)	95.0% CI for Exp (β)
						Lower	Upper
NSIP pattern	-12.70	182.18	5.97	0.94	0.00	0.00	0.60E149
UIP pattern	-1.60	0.65	5.97	0.01	0.20	0.56	0.78
AGTR2 vascular	0.26	0.89	9.23	0.002	1.30	1.10	1.55
Lymphatic density	-1.20	0.25	6.92	0.008	0.297	0.122	0.73

[1] All authors designed the study, analyzed and interpreted the data and wrote the manuscript.

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Angiotensin II type 1 and 2 receptors and lymphatic vessels modulate lung remodeling and fibrosis in systemic sclerosis and idiopathic pulmonary fibrosis

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