Central neurogenic hyperventilation: Difference between revisions

Central neurogenic hyperventilation (CNH) is an abnormal pattern of breathing characterized by deep and rapid breaths at a rate of 25 breaths per minute. Increasing irregularity of this respiratory rate generally is a sign that the patient will enter into coma. It is unrelated to other forms of hyperventilation like Kussmaul's respirations. CNH is the human body's response to reduced carbon dioxide levels in the blood, caused by contraction of cranial arteries from damage caused by lesions in certain areas of the brain stem. However, the mechanism by which CNH arises as a result from these lesions is still very poorly understood. CNH remains an underdeveloped area of medicine that needs to be explored.

Background/Overview

Discovery

Central neurogenic hyperventilation (CNH) is an extremely rare neurological disorder that was initially reported by Fred Plum, MD and August G. Swanson, MD, in 1959.^[1][2][3] Plum and Swanson described the symptoms of nine comatose patients, defining CNH as a syndrome primarily comprised of elevated arterial oxygen tension, decreased arterial carbon dioxide tension, and progressivetachypnea. These conditions lead to hypocarbia and respiratory alkalosis, which elevates blood pH.^[1][2] These symptoms occurred in the marked absence of any cardiac or pulmonary disorders that may have stimulated a compensatory increase in depth and rate of breathing that could be misdiagnosed as CNH.^[1][2][3]

The pathophysiology of the nine patients was determined by postmortem examination of the patients’ brains. Plum and Swanson reported necrosis of the central pons in five of the nine patients, and indirect compression of the pons in one additional patient.^[2][3] Their initial findings suggested that lesions in the medial pontine tegmentum leads to a disruption of cortical inhibitory effects of medullar respiratory center. Plum and Swanson suggested that failure to inhibit the activity of this particular region of the brain results in continuous stimulation of the respiratory center by the lateral pontile reticular formulation and laterally located descending neural pathway. The destruction of this required negative feedback mechanism causes the uncontrollable hyperventilation associated with CNH.^[2][3][4][5]

Additional Findings

Subsequent findings revealed CNH can also occur in conscious patients. The condition is considered extremely uncommon, and only 21 cases additional cases of tumor-inducing CNH were reported up until 2005.^[3][4] Only five of these cases were reported in children.^[3][5] The causes associated with conscious CNH are more varied than originally predicted by Plum and Swanson’s study of comatose patients, although the most commonly reported causes of CNH involve infiltrative gliomas and lymphomas of the brainstem and pons.^[3]

Although the majority of CNH-inducing tumors are located in close proximity to other medullary homeostatic centers, the psychological changes associated with CNH are restricted to alterations in the control of breathing. Most patients present with normal readings for heart rate and blood pressure, even in the case of severe alkalosis caused by CNH, which indicates that the respiratory center affected by CNH is more sensitive to compression than other areas of the brain.^[6]

Diagnosis

For the clinical diagnosis of CNH, it is essential that the symptoms, particularly respiratory alkalosis, persist while the patient is both awake and asleep. The presence of hyperventilation during sleep excludes any possible emotional or psychogenic causes for the sustained hyperventilation.^[7] There must also be no evidence of drug or metabolic causes, including cardiac or pulmonary disease, or recent or current use of respiration-stimulating drugs.^[1][7] While a positive diagnosis of CNH in adult cases should be reserved only until all other possible causes of tachypnea have been eliminated, CNH should be suspected in any alert child presenting with unexplained hyperventilation and hypocarbia leading to respiratory alkalosis.^[3] Once CNH is determined to be a possible cause of hyperventilation, lesions and their location in the brain are verified using magnetic resonance imaging (MRI).

Prognosis

The onset of CNH in all patients regardless of age can be a precursor to ensuing deterioration in patients with infiltrative tumors of the brainstem and medulla. These patients experience prolonged series of CNH before succumbing to the associated deterioration of medullary cardiovascular center, which ultimately results in death.^[3] In addition to clinical consequences of a positive CNH diagnosis, sustained hyperventilation also has a marked affect on daily life activities, and may significantly impede a patient’s ability to eat or talk. The persistent hypocarbia, alkalotic pH, and resultant electrolyte disequilibrium may also alter a patient’s mood or mental state. Patients presenting with CNH are often are described as inattentive and anxious.^[3]

Causes of CNH

Determining the exact cause of CNH has proven to be difficult, specifically because only 21 additional cases have been reported since Plum and Swanson’s initial report of the condition in 1959.^{[4] [3]} These subsequent reports deal only with conscious patients presenting with CNH, though the varied pathophysiologies present in each individual patient makes it nearly impossible to implicate either a particular structural lesion or the destruction of a specific locus as the sole cause of CNH.^[4][3].^[1] Compilations of the reports, however, have led to generalized conclusions about the primary role of structural lesions in the initiation of both juvenile and adult cases of CNH.

Tumor-Induced CNH in Adults

The majority of adult patients experiencing CNH have clinical histories of infiltrative, expanding tumors of the cortex, primarily involving the brainstem. Over three-quarters of the cases reported since the discovery of CNH by Plum and Swanson had tumors clearly involving the pons, with specific consideration given to pathology of the pontine tegmentum.^[4] CNH was also reported in patients with tumors affecting the medulla oblongata.^[3][4]

Though a diagnosis of CNH is rarely considered without evidence of brainstem infiltration, there have been other reported cases of CNH not directly involving the pons or medulla. CNH was also reported in cases involving a frontal lobe tumor, an invasive laryngeal carcinoma compressing the midbrain, an extension of tumors of the head and neck into the base of the brain, and thalamic hemorrhage.^[3][4][6] The manifestation of CNH in patients with these non-brainstem related disorders leads to greater debate about the pathophysiology of CNH and the role of other parts of the brain in the regulation of respiration.^[3][4] At this time, there have been no reported cases of CNH associated with stroke.^[4]

In each case, the nature of the tumor varied, though the two main categories of tumor were classified as either cerebral lymphomas or solid tumors, such as pontine gliomas, anaplastic medulloblastoma, or astrocytomas.^[3]

Particular attention is given to the high incidence of cerebral lymphomas associated with adult CNH. Intracerebral B-cell lymphoma represents less than 1% of all primary malignant tumors of the central nervous system.^[1][3][5] Infiltration of lymphoma cells into the pons and medulla is the most frequently reported cause of CNH, accounting for half of all CNH-inducing brain tumors, despite its considerable rarity. It has been suggested that these lymphomas are capable of diffusely penetrating the midbrain, without majorly destructing the overall structures. ^[3]

Tumor-Induced CNH in Children

CNH in children is considerably less common, and only five of the twenty one cases have been documented in children aged 11 and younger. ^[3][5] The primary difference between juvenile and adult cases of CNH is the structural identity of the tumors leading to CNH symptoms. Four of the five cases of CNH involving children were associated with solid infiltrative gliomas on the brainstem, while only one case was associated with an apparent lymphoma referred to as microgliomatosis.^[3]

Non-tumor Induced CNH

There have been only a few reported cases of non-tumor induced CNH, most of which have been successfully treated. Recently, the anticonvulsant drug Topiramate induced temporary CNH in patients, which abated after drug use was terminated.^[3] Additionally, there has been one reported case of CNH in a patient suffering from multiple sclerosis with brainstem lesions. The CNH was considered reversible and was successfully treated with high-dose intravenous methylprednisolone and plasma exchange.^[7]

Symptoms

Symptoms of CNH have been observed to vary according to the progression of CNH. The initial symptoms of CNH include a low arterial partial pressure of carbon dioxide, a high or normal arterial partial pressure of oxygen, high arterial pH, and tachypnea.^{[3][4][5][8][9]} The partial pressure of carbon dioxide has been noted by Yushi et al. to drop as low as 6.7 mmHg, while oxygen saturation remains at 99-100%.^[8] Respiratory alkalosis is induced in people affected with CNH, which stimulates the hyperpnea to attempt to compensate the rise the blood’s pH.^[5] The hyperventilation of CNH patients persists during sleep.^[5][8] Those affected have been observed to not be able to voluntarily control their breathing in order to slow it down^[3] and the hyperventilation is predominantly controlled by the diaphragm.^[8]

CNH has been found to affect people of all ages, ranging from children at the age of seven^[3] to adults at the age of eighty-seven.^[4] It has affected people while they have been both conscious and unconscious. After Plum and Swanson's initial discovery of CNH it was thought that CNH was rare in conscious patients. More cases of CNH have been observed in conscious patients since then. Additional symptoms of conscious CNH include loss of appetite, difficulty concentrating, poor memory, difficulties in eating or talking, cachexia, vomiting, disorientation, and a generalized confused state that varies from patient to patient.^{[3][4][5][8][9]} All of these symptoms are not present in each reported case of CNH, and symptoms seems to vary on a case to case basis. Other symptoms that have been associated with CNH are transient epileptic episodes with a temporary loss of consciousness. This condition is thought to result from severe hypocapnia that induces blood vessels in the brain to constrict, leading to brain ischemia.^[5] Other symptoms caused by CNH are electrolyte dysequilibrium and mood changes that primarily include anxiety due to the hyperventilation.^[3][8]

Once CNH is diagnosed, the condition generally progresses until the patient becomes unconscious or lapses into a coma. Most patients are seen to enter this state two to three months after the onset of CNH.^[3][5][8] Lange et al. cited a patient that experienced pulmonary edema, bronchitis, and pneumonia prior to death, though all reported cases of CNH describe various progressions of the condition until it worsens to the point of death.

Associations with Body Systems

CNH is most commonly associated with the central nervous system, and the majority of CNH cases have been associated with infiltrative tumors in the pons.^{[3][5][4][8][9]} Some cases involve the medulla and other regions of the brain. Primarily, researchers believe that the tumors infiltrate the pontine respiratory centers and central chemoreceptors.^[5] CNH has not been found to be associated with any other of the body’s systems. Cardiac, pulmonary, and metabolic disorders have been ruled out as causes of the hyperventilation.^[5] Tests such as electrocardiograms, echocardiograms, torso computed tomographic scans, and chest radiographs have revealed that the pulmonary and cardiac systems of CNH are normal.^[4] Liver and kidney functions are also normal.^[4] Lymph node and thyroid enlargement also have not been detected. ^[8] Association with the cardiovascular system is seen when the brain tumors reach the medullary cardiovascular centers, at which point the patient usually succumbs to death.^[3][8]

Pathophysiology

Although CNH is typically characterized by the presence of lesions in the brainstem region, the mechanism by which these lesions create uninhibited stimulation of the expiratory and inhalatory centers is still poorly understood. These lesions typically arise after cancerous cells from another location of the body metastasize and move to the brain. The mechanism by which CNH was originally thought to occur involved the separation of the pontine and medullary respiratory centers by infiltrative tumors. Animal models mimicking this separation, however, do not exhibit CNH.^[4] A secondary postulated mechanism by which CNH may function is that the lesions produce lactate which consequently serves as a stimulator for the chemoreceptors of the medullary region of the brainstem. Previous studies of CNH patients have verified the presence of lactic acid in cerebral spinal fluid.^[10]

Treatment

There is no accepted current course of treatment for CNH. Morphine is typically used for its ability to depress respiratory rate, but has only been found to be effective in reducing CNH in some cases. Successful documentation of CNH treatment typically involves the surgical removal of the lesions, or the use of chemotherapy with corticosteriods to reduce the size of lesions in the affected area of the brain. In cases where CNH presents in children, whose conditions are typically characterized by more solid tumors, aggressive surgical and chemotherapeutic methods are highly recommended.^[3]

If treatment of the lesions is ineffective, studies have shown that intravenous fentanyl, a slow-acting narcotic, or a fentanyl patch can be used to slow respiration. In patch form, fentanyl is a good alternative to morphine therapy for its high lipid solubility and ability to be worn on the body. Narcotic treatment is largely temporary and high morbidity rates in adults and children are typically dited where lesions are not removed.^[5]

Current and Future Research

Current mechanisms by which CNH functions still remain poorly developed. In addition, a standard form of treatment has not been established to treat CNH. These characteristics make CNH an important condition that still needs to be investigated in adults and children, though the extreme rarity of the condition makes it difficult for research to successfully examine clinical cases.

References

1. Sakamo, T., Kokubo, M., Sasai, K., Chin, K. (2001). “Central neurogenic hyperventilation with primary cerebral lymphoma: A case report.” Radiation Medicine. 19: 209-213. http://www.ncbi.nlm.nih.gov/pubmed/11550722
2. Sunderrajan, E.V., Passamonte, P.M. (1984). “Lymphomatoid granulomatosis presenting as central neurogenic hyperventilation.” Chest. 86: 634-636. http://chestjournal.chestpubs.org/content/86/4/634.full.pdf+html
3. Shahar E., Postovsky S., Bennett O. (2004). “Central neurogenic hyperventilation in a conscious child associated with glioblastoma multiforme.” Pediatric Neurology. 30: 287-290. http://www.sciencedirect.com/science?_ob=ArticleURL&_udi=B6TBD-4C546D8-D&_user=521319&_rdoc=1&_fmt=&_orig=search&_sort=d&_docanchor=&view=c&_searchStrId=1065143416&_rerunOrigin=google&_acct=C000026018&_version=1&_urlVersion=0&_userid=521319&md5=5b4982c1e903896844f50e8924e4efc5
4. Tarulli, A.W., Lim, C., Bui, J., Saper, C., Alexander, M. (2005). “Central neurogenic hyperventilation: A case report and discussion of pathophysiology.” Archives of Neurology. 62:1632-1634.http://archneur.ama-assn.org/cgi/content/full/62/10/1632
5. Adachi, Y., Sano, H., Doi, M., Sato, S. (2007). “Central neurogenic hyperventilation treated with intravenous fentanyl followed by transdermal application.” Journal of Anesthesia. 21:417-419.http://www.springerlink.com/content/824387617r603276/
6. Dubaybo, B.A., Afridi, I., Hussain, M. (1991). “Central neurogenic hyperventilation in invasive laryngeal carcinoma.” Chest. 99:767-769. http://chestjournal.chestpubs.org/content/99/3/767.full.pdf+html
7. Takahashi, M., Tsunemi, T., Miyayosi, T., Mizusawa, H. (2007). “Reversible central neurogenic hyperventilation in an awake patient with multiple sclerosis.” Journal of Neurology. 254:1763-1764
8. Lange, L.S., Laszlo, G. (1965). "Cerebral tumour presenting with hyperventilation." Journal of Neurology, Neurosurgery, and Psychiatry. 28: 317-319 http://jnnp.bmj.com/cgi/reprint/28/4/317.pdf
9. Terushige, T., Miyazawa, T., Fukui, S., Otani, N., Nawashito, H., Shima, K. (2005). "Central neurogenic hyperventilation in a conscious man with CSF dissemination from a pineal glioblastoma." Journal of Clinical of Neuroscience. 12:834-837. http://www.sciencedirect.com/science?_ob=ArticleURL&_udi=B6WHP-4H6X87H-B&_user=521319&_rdoc=1&_fmt=&_orig=search&_sort=d&_docanchor=&view=c&_acct=C000026018&_version=1&_urlVersion=0&_userid=521319&md5=4466519f07ae32ce9486bf47e9744b44
10. Gaviana, P., Gonzalez, J., Zhu, J., Batchelor, T.T., Henson, J.W. (2005). “Central neurogenic hyperventilation and lactate production in brainstem glioma.” Neurology. 64: 166-167. http://www.neurology.org/cgi/reprint/64/1/166

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