Jump to content

Horner's syndrome

From Wikipedia, the free encyclopedia

This is an old revision of this page, as edited by Just-a-can-of-beans (talk | contribs) at 23:29, 4 January 2024 (Pathophysiology). The present address (URL) is a permanent link to this revision, which may differ significantly from the current revision.

Horner's syndrome
Other namesBernard-Horner syndrome (BH), oculosympathetic palsy
Left-sided Horner's syndrome
SpecialtyNeurology Edit this on Wikidata

Horner's syndrome, also known as oculosympathetic paresis,[1] is a combination of symptoms that arises when a group of nerves known as the sympathetic trunk is damaged. The signs and symptoms occur on the same side (ipsilateral) as it is a lesion of the sympathetic trunk. It is characterized by miosis (a constricted pupil), partial ptosis (a weak, droopy eyelid), apparent anhidrosis (decreased sweating), with apparent enophthalmos (inset eyeball).[2]

The nerves of the sympathetic trunk arise from the spinal cord in the chest, and from there ascend to the neck and face. The nerves are part of the sympathetic nervous system, a division of the autonomic (or involuntary) nervous system. Once the syndrome has been recognized, medical imaging and response to particular eye drops may be required to identify the location of the problem and the underlying cause.[3]

Signs and symptoms

Signs that are found in people with Horner's syndrome on the affected side of the face include the following:

Interruption of sympathetic pathways leads to several implications. It inactivates the dilator muscle and thereby produces miosis. It inactivates the superior tarsal muscle which produces ptosis. It reduces sweat secretion in the face. Patients may have apparent enophthalmos (affected eye looks to be slightly sunken in) but this is not always the case. The ptosis from inactivation of the superior tarsal muscle causes the eye to appear sunken in, but when actually measured, enophthalmos is not present. The phenomenon of enophthalmos is seen in Horner's syndrome in cats, rats, and dogs.[5]

Sometimes there is flushing on the affected side of the face due to dilation of blood vessels under the skin. The pupil's light reflex is maintained as this is controlled via the parasympathetic nervous system.[citation needed]

In children, Horner's syndrome sometimes leads to heterochromia, a difference in eye color between the two eyes.[3] This happens because a lack of sympathetic stimulation in childhood interferes with melanin pigmentation of the melanocytes in the superficial stroma of the iris.[citation needed]

In veterinary medicine, signs can include partial closure of the third eyelid, or nictitating membrane.[citation needed]

Causes

Scheme showing sympathetic and parasympathetic innervation of the pupil and sites of a lesion in Horner's syndrome.

Horner's syndrome is usually acquired as a result of disease, but may also be congenital (inborn, associated with heterochromatic iris) or iatrogenic (caused by medical treatment). In rare cases, Horner's syndrome may be the result of repeated, minor head trauma, such as being hit with a soccer ball. Although most causes are relatively benign, Horner's syndrome may reflect serious disease in the neck or chest (such as a Pancoast tumor (tumor in the apex of the lung) or thyrocervical venous dilatation).[citation needed]

Causes can be divided according to the presence and location of anhidrosis:[citation needed]

Pathophysiology

Horner syndrome is due to a deficiency of sympathetic activity. The site of lesion to the sympathetic outflow is on the ipsilateral side of the symptoms. The following are examples of conditions that cause the clinical appearance of Horner's syndrome:[8]

  • First-order neuron disorder: Central lesions that involve the hypothalamospinal tract (e.g. transection of the cervical spinal cord).
  • Second-order neuron disorder: Preganglionic lesions (e.g. compression of the sympathetic chain by a lung tumor) that releases acetylcholine.
  • Third-order neuron disorder: Postganglionic lesions at the level of the internal carotid artery (e.g. a tumor in the cavernous sinus or a carotid artery dissection) that releases norepinephrine.
  • Partial Horner's syndrome: In case of a third-neuron disorder, anhidrosis is limited to the middle part of the forehead or can be absent, resulting in a partial Horner's syndrome.[9]

If patients have impaired sweating above the waist affecting only one side of the body, and they do not have clinically apparent Horner's syndrome, then their lesions are just below the stellate ganglion in the sympathetic chain.[citation needed]

Diagnosis

Left-sided Horner's syndrome in a cat as a result of trauma, demonstrating miosis in left pupil.

Three tests are useful in confirming the presence and severity of Horner syndrome:

  • Cocaine drop test: Cocaine eyedrops block the reuptake of post-ganglionic norepinephrine resulting in the dilation of a normal pupil from retention of norepinephrine in the synapse. However, in Horner's syndrome the lack of norepinephrine in the synaptic cleft causes mydriatic failure. A more recently introduced approach that is more dependable and obviates the difficulties in obtaining cocaine is to apply the alpha-agonist apraclonidine to both eyes and observe the increased mydriatic effect (due to hypersensitivity) on the affected side of Horner syndrome (the opposite effect to what the cocaine test would produce in the presence of Horner's).[8]
  • Paredrine test: This test helps to localize the cause of the miosis. If the third order neuron (the last of three neurons in the pathway which ultimately discharges norepinephrine into the synaptic cleft) is intact, then the amphetamine causes neurotransmitter vesicle release, thus releasing norepinephrine into the synaptic cleft and resulting in robust mydriasis of the affected pupil. If the lesion itself is of the third order neuron, then the amphetamine will have no effect and the pupil remains constricted. There is no pharmacological test to differentiate between a first and second order neuron lesion.[9]
  • Dilation lag test[clarification needed]

It is important to distinguish the ptosis caused by Horner's syndrome from the ptosis caused by a lesion to the oculomotor nerve. In the former, the ptosis occurs with a constricted pupil (due to a loss of sympathetics to the eye), whereas in the latter, the ptosis occurs with a dilated pupil (due to a loss of innervation to the sphincter pupillae). In a clinical setting, these two ptoses are fairly easy to distinguish. In addition to the blown pupil in a CNIII (oculomotor nerve) lesion, this ptosis is much more severe, occasionally occluding the whole eye. The ptosis of Horner syndrome can be quite mild or barely noticeable (partial ptosis).[8]

When anisocoria occurs and the examiner is unsure whether the abnormal pupil is the constricted or dilated one, if a one-sided ptosis is present then the abnormally sized pupil can be presumed to be on the side of the ptosis.[citation needed]

History

The syndrome is named after Johann Friedrich Horner, the Swiss ophthalmologist who first described the syndrome in 1869.[10][11] Several others had previously described cases, but "Horner's syndrome" is most prevalent. In France and Italy, Claude Bernard is also eponymized with the condition (Claude Bernard–Horner syndrome, abbreviated CBH[12]). In France, Francois Pourfour du Petit is also credited with describing this syndrome.

Children

The most common causes in young children are birth trauma and a type of cancer called neuroblastoma.[13] The cause of about a third of cases in children is unknown.[13]

See also

References

  1. ^ "Horner syndrome: MedlinePlus Medical Encyclopedia". medlineplus.gov. Retrieved 2019-05-06.
  2. ^ Reference, Genetics Home. "Horner syndrome". Genetics Home Reference. Retrieved 2019-05-06.
  3. ^ a b c Ropper AH, Brown RH (2005). "14: disorders of ocular movement and pupillary function". In Ropper AH, Brown RH (eds.). Adams and Victor's Principles of Neurology (8th ed.). New York: McGraw-Hill Professional. pp. 222–45. ISBN 0-07-141620-X.
  4. ^ a b c d e f g "Horner's syndrome | Genetic and Rare Diseases Information Center (GARD) – an NCATS Program". rarediseases.info.nih.gov. Retrieved 2019-10-15.
  5. ^ Daroff R (April 2005). "Enophthalmos is not present in Horner syndrome". PLOS Medicine. 2 (4): e120. doi:10.1371/journal.pmed.0020120. PMC 1087222. PMID 15839747.
  6. ^ Laing C, Thomas DJ, Mathias CJ, Unwin RJ (October 2000). "Headache, hypertension and Horner's syndrome". Journal of the Royal Society of Medicine. 93 (10): 535–6. doi:10.1177/014107680009301010. PMC 1298129. PMID 11064693..
  7. ^ Pitton Rissardo, Jamir; Fornari Caprara, Ana Letícia (2019-03-07). "Isolated horner syndrome secondary to eagle syndrome". Neurology and Clinical Neuroscience. 7 (3): 156–157. doi:10.1111/ncn3.12279. ISSN 2049-4173. S2CID 86557308.
  8. ^ a b c Koka, Kirthi; Patel, Bhupendra C. (2023), "Ptosis Correction", StatPearls, Treasure Island (FL): StatPearls Publishing, PMID 30969650, retrieved 2024-01-04
  9. ^ a b Lee JH, Lee HK, Lee DH, Choi CG, Kim SJ, Suh DC (January 2007). "Neuroimaging strategies for three types of Horner syndrome with emphasis on anatomic location". AJR. American Journal of Roentgenology. 188 (1): W74-81. doi:10.2214/AJR.05.1588. PMID 17179330.
  10. ^ Horner JF (1869). "Über eine Form von Ptosis". Klin Monatsbl Augenheilk. 7: 193–8.
  11. ^ synd/1056 at Who Named It?
  12. ^ Logan, Carolynn M.; Rice, M. Katherine (1987). Logan's Medical and Scientific Abbreviations. J. B. Lippincott and Company. pp. 58. ISBN 0-397-54589-4.
  13. ^ a b Kennard C, Leigh RJ (2011-06-28). Neuro-ophthalmology: Handbook of Clinical Neurology (Series Editors: Aminoff, Boller and Swaab). Elsevier. p. 452. ISBN 9780702045479.