Immunohistochemical analysis of apoptosis and cell proliferation in lungs of premature infants with chronic lung disease (bronchopulmonary dysplasia)

Witkowski, Sandra Mara; Noronha, Lúcia de; Okamoto, Cristina T.; Oldenburg Neto, Carlos F.; Almeida, Tammy; Nagashima, Seigo; Bahr, João A.

doi:10.5935/1676-2444.20160064

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PATHOLOGY, Original article • J. Bras. Patol. Med. Lab. 52 (6) • Nov-Dec 2016 • https://doi.org/10.5935/1676-2444.20160064 copy

Immunohistochemical analysis of apoptosis and cell proliferation in lungs of premature infants with chronic lung disease (bronchopulmonary dysplasia)

Análise imuno-histoquímica da apoptose e proliferação celular em pulmões de prematuros com doença pulmonar crônica (displasia broncopulmonar)

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

Introduction:

The pathophisiology of chronic lung disease (CLD), clinically known as bronchopulmonary dysplasia is not clear. It is believed that protective mechanisms, such as the release of inflammatory mediators and the activation of apoptotic and/or proliferative processes are activated in the lung tissue of premature infants in an attempt to repair tissue injury caused by exposure to oxygen and mechanical ventilation.

Objective:

Assess the presence of apoptosis and cell proliferation in the lungs of premature infants with CLD, exposed to oxygen and/or mechanical ventilation, by analyzing the proteins expression: proliferating cell nuclear antigen (PCNA), phosphatase and tensin homolog (PTEN), B-cell lymphoma 2 (Bcl-2), tumor necrosis factor receptor family member (Fas), fas-associated protein with death domain (FADD), tumor necrosis factor receptor type 1-associated death domain protein (TRADD), Caspase 3 and Caspase 8.

Material and methods:

We analyzed 32 infants autopsies at gestational age of less than 34 weeks exposed to oxygen therapy. The study was divided into three groups: "classic" CLD, "new" CLD and "without" CLD. Immunohistochemical analysis was performed.

Results and discussion:

A higher proliferation rate was observed in infants with CLD suggesting that longer exposure to mechanical ventilation may stimulates cell proliferation. The PTEN and Caspase 8 expressions were higher in the "new" CLD group, compared to the "without" CLD group, indicating that the "new" CLD form is more susceptible to apoptosis.

Conclusion:

Apoptosis and cell proliferation are involved in the pathophisiology of CLD. The "new" CLD form is more susceptible to apoptosis, while cell proliferation is more evident in the groups with CLD.

Key words:
apoptosis; pharmacological biomarkers; cell proliferation; bronchopulmonary dysplasia; neonatology

	Classic CLD (n = 11)	New CLD (n = 5)	Without CLD (n = 16)	p-value
Pathological characteristics	Hyaline membrane, interstitial fibrosis and over-distended acini	Slight septal edema, low-grade inflammation	Slight septal edema, low-grade inflammation
Morphometry (number of alveoli)^* * mean μm2/standard deviation;	-	40.94/15.13	55.8/15.1	0.050^a a nonparametric Mann- Whitney test, p < 0.05.
Morphometry (alveolar perimeter)^* * mean μm2/standard deviation;	^-	481.52/182.42	560.4/168.8	0.548^a a nonparametric Mann- Whitney test, p < 0.05.

Parameters	Classic CLD	New CLD	Without CLD
Gender
Female	6	4	11
Male	5	1	5
Birth weight^* * mean/standart deviation; (g)	1021/289	1340/398	959/358
Gestational age (weeks)^* * mean/standart deviation; ^b b p = 0.005.	32/3.3	33.4/3.1	28.8/2.6
Apgar score first minute^* * mean/standart deviation; (n =29/32)^† † number of cases;	2.6/2	6/3.5	3.5/2.7
Apgar score fifth minute^* * mean/standart deviation; (n =29/32)^† † number of cases;	6.2/2.6	8.4/1.9	5/3.5
Pregnancy hypertension event (n = 31/32)^† † number of cases;
Yes	3	3	2
No	8	2	13
Gestational diabetes (n =32/32)^† † number of cases;
Yes	0	1	0
No	11	4	16
Chorioamnionitis (n =32/32)^† † number of cases;
Yes	1	0	2
No	10	5	14
Amniotic sac disruption (n= 27/32)^† † number of cases;
Yes	1	1	4
No	9	4	8

Parameters	Classic CLD (n = 11)	New CLD (n = 5)	Without CLD (n = 16)	p-value
Patent ductus arteriosus
Yes	10	2	2	0.0003^ Pearson test;
No	1	3	14	0.0003^ Pearson test;
Antibiotic therapy
Yes	10	4	8	> 0.017^‡ ‡ Fisher test, p > 0.017 (adjusted for Bonferroni);
No	1	1	8
Surfactant therapy
Yes	7	0	1	0.0089
No	4	5	15	0.0089
Necrotizing enterocolitis
Yes	7	2	1	0.002^‡ ‡ Fisher test, p > 0.017 (adjusted for Bonferroni);
No	4	3	15	0.002^‡ ‡ Fisher test, p > 0.017 (adjusted for Bonferroni);
Bronchopneumonia
Yes	6	0	1	0.009^‡ ‡ Fisher test, p > 0.017 (adjusted for Bonferroni);
No	5	5	15	0.009^‡ ‡ Fisher test, p > 0.017 (adjusted for Bonferroni);
Pulmonary hemorrhage
Yes	3	1	1	> 0.017^‡ ‡ Fisher test, p > 0.017 (adjusted for Bonferroni);
No	8	4	15
Pulmonary hypertension
Yes	2	1		> 0.017^‡ ‡ Fisher test, p > 0.017 (adjusted for Bonferroni);
No	9	4	0 16
Intracranial hemorrhage
Yes	4	2	1	> 0.017^‡ ‡ Fisher test, p > 0.017 (adjusted for Bonferroni);
No	7	3	15
Sepsis
Yes	11	4	3	0.001^‡ ‡ Fisher test, p > 0.017 (adjusted for Bonferroni);
No	0	1	13	0.001^‡ ‡ Fisher test, p > 0.017 (adjusted for Bonferroni);
Corrected gestational age (weeks)^* * mean/ standart deviation;
	32/3.3	33.4/3.1	28.8/2.6	0.005^§ § Kruskal-Wallis nonparametric test (p < 0.05).
Survival time (days)^* * mean/ standart deviation;
	23.4/12.3	12.4/5.5	1.4/1.6	< 0.001^§ § Kruskal-Wallis nonparametric test (p < 0.05).
Asphyxia
Yes	6	1	9	> 0.017^‡ ‡ Fisher test, p > 0.017 (adjusted for Bonferroni);
No	5	4	7

	Classic CLD	New CLD	Without CLD
Days of mechanical ventilation^* * mean/ standart deviation.	12.90/9.23	3.4/3.91	1.33/1.69
Days of CPAP^* * mean/ standart deviation.	5.6/7.66	4.4/3.2	1.91/1.63
Days of oxygen tent^* * mean/ standart deviation.	3.8	1.8	0
Days of oxygen catheter^* * mean/ standart deviation.	0.27	0.8	0
FiO₂ Max (%)^* * mean/ standart deviation.	95/12.24	85/30	98.75/7.07
PIP Max (mmHg)^* * mean/ standart deviation.	21.16/3.37	20/0	23.18/6.98
PEEP Max (mmHg)^* * mean/ standart deviation.	4.7	5	5.05
Days of oxygen therapy/survival time^* * mean/ standart deviation.	21.36/12.26	10.4/2.79	1.4/1.6

Protein	Classic CLD (n = 11) m/SD	New CLD (n = 5) m/SD	Without CLD (n = 16) m/SD	p-value^§ § Kruskal-Wallis nonparametric test (p < 0.05).
PCNA septal (n = 26/32)^* * number of positive cells;	69.1/55.8	61.5/38.1	24.2/40.5	0.057
PCNA alveoli (n = 26/32)^* * number of positive cells;	4.59/3.63	3.25/1.55	3.21/5.55	0.246
Bcl-2 degree	2.18/1.83	1.8/1.79	0.94/1.61	0.236
Bcl-2 pattern	2.18/1.83	2.18/1.83	0.88/1.45	0.196
PTEN degree^* * number of positive cells; (n = 29/32)^* * number of positive cells;	4.67/2	7.5/1	3.63/2.39	0.015
PTEN pattern^* * number of positive cells; (n = 29/32)^* * number of positive cells;	5.78/3.15	8.75/3.95	5/3.86	0.2
Fas^a a immunopositive area (%/SD);	0.032/2289.2	0.039/4650.9	0.030/2483.3	0.967
FADD^a a immunopositive area (%/SD);	0.028/2476.3	0.024/1073.5	0.104/3425.1	< 0.001
Caspase 3^a a immunopositive area (%/SD);	0.012/777.3	0.012/1060.5	0.014/1235	0.993
Caspase 8^a a immunopositive area (%/SD);	0.031/589	0.046/951.7	0.032/766.3	0.010

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[1] Corresponding author: Lúcia de Noronha e/ou Sandra Mara Witkowski, Pontifícia Universidade Católica do Paraná; Escola de Medicina; Laboratório de Patologia Experimental, Rua Imaculada, Conceição, 1.155; Prado Velho, CEP: 80215-901; Curitiba-PR, Brasil. e-mail: lnno@terra.com.br e/ou sandrawtk@gmail.com