CASE STUDY: PATIENT WITH ALVEOLAR PROTEINOSIS

S P Wessels*

SUMMARY

Alveolar proteinosis is a rare disease of unknown etiology in 
which the alveoli are filled with lipid-proteinaceous material. The 
diagnosis is usually made on an open lung biopsy. The main 
symptoms are chest pain, tiredness, persistent pyrexia and a 
productive cough with purulent, bloodstained sputum. Exertion 
dyspnoea, however, is regarded as the most important symp­
tom. Chest X-rays demonstrate a picture similar to severe pul­
monary oedema. The lung functions and the blood gases are 
indicators of the severity of the disease and there Is usually a 
reduction in the vital capacity, S a 0 2 and Pa02.
A case study of a patient with this diagnosis treated atTygerberg 
Hospital is reported. He was admitted complaining of the above 
mentioned symptoms, his lung functions and blood gases were 
extremely poor and the chest X-rays showed bilateral diffuse 
opacifications. He had to be ventilated with high percentages of 
oxygen and a high PEEP to maintain an adequate S a 0 2 and 
Pa02. The infection was treated with antibiotics and corticoste­
roids. Because of the presence of a tremendous amount of 
bronchial secretions, chest physiotherapy was very important. 
General techniques used were bagging, percussion and shak­
ing in alternative side-lying and were combined with Mista- 
bron:Saline inhalations to help dissolve the proteinaceous 
material in the alveoli. Over a period of 8 weeks he recovered 
remarkably, but two months after admission his condition unex­
pectedly deteriorated and he died three days later.

OPSOMMING

Alveoldre protei'enose is 'n baie rare siekte van onbekende 
oorsaak waarin die alveoli gevul is met lipied-proteTenagtige 
materiaal. Die diagnose word gewoonlik met behulp van 'n oop 
longbiopsie gemaak. Die mees algemene simptome is borskas- 
pyn, moegheid, sweet en 'n produktiewe hoes met purulente, 
bloedbevlekte sputum. Inspanningsdispnee word as die belan- 
grikste simptoom beskou. Die borskas X-strale stem ooreen met 
die van ernstige pulmonale edeem. Die longfunksies en die 
bloedgasse dul die ems van die siekte aan en daar is gewoonlik 
’n vermindering van die longvervormbaarheid, S a 0 2 en Pa02. 
’n Gevalstudie van 'n pasignt met di6 diagnose wat in Tygerberg 
Hospitaal behandel is, word hier beskryf. Sy simptome by op­
name het met die tipiese beeld ooreengestem, die longfunksies 
en bloedgasse was baie swak en die borskas X-strale het 
bilaterale diffuse versluierings getoon. Hy het ventilasie met hod 
PEEP benodig om ’n aanvaarbare S a 0 2 en Pa02 te handhaaf. 
Die infeksie is met antibiotika en kortikosterolede behandel. As 
gevolg van die groot hoeveelheid brongiale sekresies was bor­
skas fisioterapie baie belangrik. Algemene tegnieke gebrulk was 
manuele hiperinflasie, beklopping en skud in alternatiewe sylS 
en dit is gekombineer met Mistabron.Saline inhalasies om te 
help met die oplossing van die protelenagtige materiaal in die 
alveoli. Oor ’n tydperk van 8 weke het die pasiSnt merkwaardig 
herstel, maar twee maande na opname het sy toestand egter 
onverwags verswak en hy is drie dae later oorlede.

INTRODUCTION
Alveolar proteinosis is a very rare disease o f unknown etiology 

in which the alveoli are filled with lipid-proteinaceous material.1 The 
disease was first described by Rosen et al in 1958 and the material 
from the first patient was obtained at lung biopsy in July 1953 at 
Massachusetts General Hospital.2 During the 12 year period (1953- 
1965) only 85 cases (the original histological criteria of Rosen et al 
have been adhered to in all the recorded cases) have been reported 
in the literature,3 giving some indication of the rarity of this disease. 
To date, no South African cases have been reported in the literature. 
Tygerberg Hospital (a large academic hospital in Cape Province, 
South Africa) has treated only 5 cases during the period 1975-1989.4

HISTORY
There is usually a history of exposure to dust -  especially silica 

dust.2 According to Larson and Gordiner (1965) a more universal 
inhalant is tobacco smoke.3 This condition is three times more com­
mon in men than in women and can affect persons of any age but is 
uncommon in neonates and infants.5 In most cases it is difficult (or 
impossible) to establish the exact time of onset of the pulmonary 
disease. Almost half of the patients in Rosen’s study had premonitory 
febrile illnesses that were considered to be pneumonia.2

DIAGNOSIS
The diagnosis can only be made on a microscopic examination 

of the sputum, an open lung biopsy or bronchial lavage.5

PATHOLOGY
The disease results from an initial type 2 granular pneumocyte 

hyperplasia which causes excessive production of a phospholipid 
material combined with protein, similar to surfactant but lacking its 
surface-tension-reducing properties. This overwhelms the phagocytic 
potential of the alveolar phagocytes. The result is an accumulation 
within the alveolar lumen as well as within intra-alveolar macrophages 
of the phospholipid material which both fills it and destroys it as an 
effective aerating unit. According to Heppleston et al (1972)6 there 
is no evidence to support the view that the alveolar macrophages lack 
their normal mobility, but Corrin et al (1970)7 said that once the 
macrophages become distended with lamellar lipids they round up 
and their mobility is seriously impaired. Alveolar lipoproteinosis does 
not result from disordered bronchiolar and bronchial clearance 
mechanisms. There is also no evidence that it is due to Pneumocystis 
carinii infections.6

Microscopically the respiratory bronchioles and alveolar walls 
are usually of normal thickness but may be slightly thickened due to 
a mainly lymphocytic infiltration. The alveoli are lined by flattened 
epithelial cells which, in more chronic cases, may partially o r com­
pletely disappear. The lining cells secrete the proteinaceous material 
which fills the alveoli and some of the respiratory bronchioles. This is 
the most striking feature of the disorder.,7

SYMPTOMS
The disease may be asymptomatic and only suspected after 

routine chest X-rays. Other symptoms include complaints o f chest

* S P Wessels, BSc (Hons) Physiotherapy, University of Stellenbosch 
Contact address: (ite S P Wessels, P O Box 63, Tygerberg 7505

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pain, tiredness, persistent pyrexia and a productive cough with puru­
lent, bloodstained sputum. The most common symptom is one of 
exertion dyspnoea.2' ’5

CHEST X-RAYS
Chest X-rays show a fine, diffuse, perihilar, radiating, vaguely 

nodular “butterfly” distribution as also seen in severe pulmonary 
oedema.iSA* The clue to the diagnosis is the inappropriateness o f the 
symptomatology in view of this appearance, When resolution occurs, 
the lesions seem to disappear, beginning peripherally and progressing 
towards the hilus. In some cases, however, they become increasingly 
radiopaque focally, suggesting deposition of fibrous connective tissue. 
Absence of significant enlargement of the hilar nodes as in the case 
of sarcoidosis is characteristic of alveolar proteinosis.2

LUNG FUNCTIONS
Lung functions and blood gases are the indicators of the severity 

of the disease. There is a reduction in the vital capacity and com­
pliance and also of the oxygen uptake, which leads to a reduction of 
the SaC>2 at rest. There is also a reduction of the PaC>2 because of the 
increased right-to-left shunt.U3,s Interpretation of these findings has 
been generally that of a restrictive type of ventilatory defect with 
impairment of diffusion and a venous-arterial admixture.8

LABORATORY DATA

While there is no evidence of anaemia, there may be a tendency 
to polycythaemia (high red cell count, raised hemoglobin). Leucocy- 
tosis is the result of an infection superimposed on the underlying 
pathology but varies from normal to as high as

20 000/mm2.5’9

COURSE
In the absence of an infection the prognosis varies and in about 

50% of the cases there is a partial or complete spontaneous remission. 
Interstitial fibrosis may supervene in longstanding cases and choles­
terol crystal aggregations are found. The course of the disease is 
uninfluenced by steroid or antibiotic therapy.

CASE REPORT
A 24 year old man from the Defence Force presented with a 5 

month history of dyspnoea, chest pain, sleeplessness, loss of appetite, 
weight loss and a productive cough with purulent, bloodstained spu­
tum. There was no known exposure to any industrial toxins and no 
history o f lung or cardiovascular disease. Two weeks before admission 
a country general practitioner diagnosed pneumonia.

On admission in the respiratory intensive care unit at Tygerberg 
Hospital he had tachypnoea (36/min), tachycardia (130/min), bilat­
eral crackles and was in respiratory failure (Pa0 2  =  6,1; PaCo2 = 
5 ,0 ). The chest X-rays showed bilateral diffuse opacifications. An 
initial differential diagnosis of interstitial lung disease was made.

COURSE AND MEDICAL TREATMENT
The patient was initially treated on a 40% oxygen CPAP-mask. 

His blood gases worsened and on the day after admission he was 
intubated and ventilated with a Servo ventilator (F 1 O2 = 0,6; V j  = 
782 ml; T /T W  = 15/15; PEEP =  10cm H 2O; with a peak pressure of 
50 cm H 2O. He was very restless and had to be sedated and relaxed. 
An open lung biopsy was performed on the third day and a diagnosis 
of alveolar proteinosis made. On day 7 a left pneumothorax was 
diagnosed and an underwater drain inserted. A tracheostomy was 
performed the following day.

To help dissolve the proteinaceous material in the alveoli, 4% 
Lichnocaine (7,5 ml):70% Alcohol (7,5 ml) inhalations were begun 
on day 5 but were stopped 5 days later. Joubert4 states that Lichno- 
caine:Alcohol inhalations would have had to be given for at least 3 
weeks to be effective and therefore, in this application, cannot be

regarded as therapeutic. One week after admission Mistabron (2 
ml):Saline (2 ml) inhalation was started in conjunction with chest 
physiotherapy and the proteinaceous material was successfully dis­
solved.

Five weeks after admission fever spikes developed and for the 
first time lung abscesses were suspected. Five days later he developed 
a left-sided bronchopleural fistula. The bronchopleural fistula began 
to drain pus twenty days later and an abscess was again suspected. 
Bronchopneumonia was also now suspected.

The patient had to be ventilated on high percentages of oxygen 
and a high PEEP for a long time to maintain efficient ventilation and 
adequate blood gases. However, he improved so much that he could 
be put on a 30% oxygen Blue Blower two months after admission. A 
Negus tube could be put in two days later, but this led to increased 
sputum production. The tracheostomy tube had to be inserted again 
and the patient reconnected to the CPAP system. The nature of the 
secretions again suggested a lung abscess.

The chest X-rays on day 67 showed a big abscess in the left lower 
lobe which probably drained through the lung. Late that evening he 
became acutely dyspnoeic and cyanotic. A right pneumothorax was 
diagnosed and underwater drain inserted. He was again ventilated. 
The next day bilateral bronchopleural fistulas were diagnosed and a 
large amount of secretions were produced. His condition worsened 
and the blood gases were poor.

The afternoon of the following he had a cardiopulmonary arrest 
and resuscitation was not successful.

Gas E x c h a n g e

Measurement 
—  P a 0 2  —  S a02 PaC02

Fi 1. Variations in gas exchange 28/9/89 to 3/11/89

H a e m a t o l o g y  R es ul ts

• WCC —  RCC Hb

Fig 2. Haematology results

LUNG FUNCTIONS AND GAS EXCHANGE
There was a serious reduction o f compliance and adequate

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SaC>2 and PaCh could only be maintained with fairly high percentages 
of oxygen (Fig 1.)

MEDICATION
Throughout his hospitalisation the patient had leucocytosis (Fig 

2) as a result of multiple opportunistic lung infections. Depending on 
the organisms cultured, the infection was treated with different anti­
biotics. Treatment with corticosteroids was begun six weeks post-ad­
mission and resulted in dramatic improvement, casting doubt on the 
diagnosis. It was only after the microscopic post mortem that the 
diagnosis could finally be confirmed.

PHYSIOTHERAPY
The first day auscultation revealed bilateral inspiratory and 

expiratory crackles (secretions). The chest physiotherapy consisted of 
localized breathing and percussion and shaking in alternate side lying. 
As he was sedated after the intubation, the chest physiotherapy then 
consisted o f bagging, overpressure, and percussion and shaking in 
alternate side lying. On day 20 the chest X-rays showed bullae espe­
cially in the left upper lobe and the bagging was stopped. Following 
the introduction o f Mistabron:Saline inhalations he produced a great 
amount o f brown, purulent sputum. After two weeks auscultation 
revealed bronchial breathing in the anterior basal segment of the left 
lower lobe and treatment was concentrated there.

Passive movements o f his limbs and stretching of all two-joint 
muscles were included in the treatment every day.

Sedation was stopped on day 38 and the patient’s level of 
consciousness returned to normal. At that stage he was under­
standably very weak, but could start with strengthening exercises and 
9 days later he was sitting in a chair for the first time. On day 66 his 
condition deteriorated suddenly and the exercises were stopped.

POST MORTEM 

Macroscopic examination:
Lung -  Emphysema (mucoid pus). Big abscesses especially in 

the right upper lobe and the left lower lobe which drained to the 
pleural cavities.

H eart -  Mderate hypertrophy o f the left and right ventricles.
Urogenital -  Oedematous kidneys

Microscopic examination:
L ungs- Abscess, empyema, alveolar proteinosis, bronchopneu­

monia, aspiration

DISCUSSION
The main motivation for writing this article was the rareness and 

uniqueness of the disease.
While there are quite a number of similarities between the 

textbook description of the disease and the case history of this patient 
there are also some differences. It was difficult to establish the exact 
time of the onset of the pulmonary disease, and the first diagnosis was 
also one of pneumonia.

His initial symptoms of dyspnoea, chest pain, a productive 
cough and chest X-rays similar to severe pulmonary oedema, fitted 
the description of alveolar proteinosis. The open lung biopsy con­
firmed the diagnosis.

The gaseous exchange and lung fiincions were poor and during 
ventilation high percentages of oxygen (60-100%) and high PEEP 
(as high as 22 cm H 2O) were needed to maintain adequate Pa0 2  and 
Sa02. A  really effective tidal volume could never be reached due to 
the air-leak through the bronchopleural fistula.

In the case of this patient there was no evidence o f polycy- 
thaemia, and the leucocytosis (see Fig 2) was the result of severe 
infection.

Although the corticosteroids brought temporary improvement, 
they impaired the immunologic response and lowered the body’s

resistance to infection, and that probably in the end caused his death.
The chest physiotherapy was very important because of the 

tremendous amount of bronchial secretions. Daily, at both treat­
ments, he produced a copious amount of brown, purulent secretions.

When the sedation was stopped and the strengthening exercises 
began, he was very co-operative and each session was a rewarding 
experience.

Towards the end he improved so much that, three days before 
his death, we started planning a visit to the hospital garden.

The evening of day 65 his condition suddenly took a turn for the 
worse and he died two days later. Although from the start his prog­
nosis was considered poor, he improved to such an extent that his 
sudden and unexpected death was a shock.

REFERENCES
1. Sykes MK, McNicol MW, Campbell EJMRespiratory Failure. Second 

Edition, Oxford, London, Edinburgh, Melbourne: Blackwell Scientific 
Publications, 1976.

2. Rosen SH, Castleman B, Liebow AA. Pulmonary alveolar proteinosis. New
Eng J  Med 1958; 258(23): 1123-42

3. Larson RC, Gordiner R  Pulmonary alveolar proteinosis (Report of six
cases, review of literature, and formulation of a new theory). Ann Intern 
Med 1965; 62(2): 292-312

4. Joubert J R  Department Internal Medicine. University of Stellenbosch and
Tygerberg Hospital; personal communication.

5. Spencer H. Pathology o f the Lung (Volume 2). Fourth edition. Oxford, New
York, Toronto: Pergamon Press, 1985.

6. Heppleton AG, Young AE. Alveolar lipo-proteinosis: An ultrastructural
comparison of the experimental and human forms. J  Path 1972; 107(2): 
107-17

7. Corrin B, King E. Pathogenesis of experimental pulmonary alveolar pro­
teinosis. Thorax 1970; 25:230-6

8. Divertie MB, Brown AL, Harrison EG. Pulmonary alveolar proteinosis
(Two cases studied by electron microscopy). Am  J  Med 1960; 40(3): 351-9

9. Hinshaw HC, Murray JF. Diseases o f the Chest. Fourth edition. Philadel­
phia, London, Toronto: W B Sanders Comp, 1980. V

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Bladsy 14 Fisioterapie, Februarie 1991, deel 47 no 1

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