Hemoglobin Is Expressed by Alveolar Epithelial Cells

Danforth A. Newton,Richard A. Dluhy,K. Murali Krishna Rao,John E. Baatz

doi:10.1074/jbc.m509314200

Abstract

Hemoglobin gene expression in non-erythroid cells has been previously reported in activated macrophages from adult mice and lens cells, and recent studies indicate that alveolar epithelial cells can be derived from hematopoietic stem cells. Our laboratory has now produced strong evidence that hemoglobin is expressed by alveolar type II (ATII) cells and Clara cells, the primary producers of pulmonary surfactant. ATII cells are also closely involved in innate immunity within the lung and are stem cells that differentiate into alveolar type I cells. Reverse transcriptase-PCR was used to measure the expression of transcripts from the alpha- and beta-globin gene clusters in several human and rodent pulmonary epithelial cells. Surprisingly, the two major globin mRNAs characteristic of adult erythroid precursor cells were clearly expressed in human A549 and H441 cell lines, mouse MLE-15 cells, and primary ATII cells isolated from normal rat and mouse lungs. DNA sequencing verified that these PCR products were indeed the result of specific amplification of globin gene cDNAs. These alveolar epithelial cells also expressed the corresponding hemoglobin protein subunits as determined by Western blotting, and tandem mass spectrometry sequencing was used to verify the presence of both alpha- and beta-globin polypeptides in rat primary ATII cells. The function of hemoglobin expression by cells of the pulmonary epithelium will be determined by future studies, but this novel finding could potentially have important implications for the physiology and pathology of the lung.

Highlights

Hemoglobin gene expression in non-erythroid cells has been previously reported in activated macrophages from adult mice and lens cells, and recent studies indicate that alveolar epithelial cells can be derived from hematopoietic stem cells
PCR products corresponding to ␣-globin (HBA) and ␤-globin (HBB), the primary globin mRNAs expressed by erythroid precursor cells in adult mammals, were found in human cell lines A549 (ATII-like adenocarcinoma) and H441 (Clara cell-like adenocarcinoma), mouse cell line MLE-15, and alveolar type II (ATII) primary cells isolated from normal rat and mouse lungs
The usage of ATII primary cells from normal rat and mouse lungs, difficult to maintain in culture, was important because it has been reported that transformation with herpes or Rous sarcoma viruses can activate ␣-globin transcription in some cell lines [30, 31], and certain patterns of aberrant gene expression are hallmarks of most tumor cell lines

Summary

Introduction

Hemoglobin gene expression in non-erythroid cells has been previously reported in activated macrophages from adult mice and lens cells, and recent studies indicate that alveolar epithelial cells can be derived from hematopoietic stem cells. An emerging concept on the primordial function of hemoglobinlike proteins is that they protect cells against oxidative and nitrosative stress [5, 6] Despite this widespread distribution of hemoglobin-like proteins (including myoglobin, neuroglobin, and cytoglobin), it has long been thought that hemoglobin itself is expressed only in cells of erythroid lineage in adult vertebrates. We demonstrate that some types of respiratory epithelial cells of human, rat, or mouse origin, including alveolar type II (ATII) epithelial cells ( called type II pneumocytes) and Clara cells, express hemoglobin In vivo, these cells are the primary producers of pulmonary surfactant, essential for normal lung function as well as innate immunity (9 –11). Our novel finding may have enormous implications in the physiology and pathology of the lung because of the many defined roles inherent to the structures of the hemoglobin molecule and its derived peptides, including gas exchange, NO metabolism, blood pressure regulation, and protection against oxidative and nitrosative stress

Methods

Results

Conclusion