Ulnar Neuropathy due to Cubital Tunnel Syndrome Caused by Anconeus Epitrochlearis: A Case Report

Article information

Nerve. 2021;7(1):20-23
Publication date (electronic) : 2021 April 30
doi : https://doi.org/10.21129/nerve.2021.7.1.20
1Department of Neurosurgery, Seoul St. Mary’s Hospital, College of Medicine, The Catholic University of Korea, Seoul, Republic of Korea
2Catholic Neuroscience Institute, College of Medicine, The Catholic University of Korea, Seoul, Republic of Korea
Corresponding author: Byung-chul Son, MD, PhD, Department of Neurosurgery, Seoul St. Mary’s Hospital, 222 Banpo-daero, Seocho-gu, Seoul, 06591, Republic of Korea, Tel: +82-2-2258-6122, Fax: +82-2-594-4248, E-mail: sbc@catholic.ac.kr
Received 2020 October 29; Revised 2020 December 10; Accepted 2020 December 23.

Abstract

A 24-year-old, right-handed male patient presented with a 1-month history of continuous tingling paresthesia involving left medial hand and fingers accompanied by clumsiness of left hand and fingers. The-pain onset was sudden and marked by a severe aching pain in the medial elbow and medial scapular areas, without any prior cause. Two weeks of excruciating pain led to clumsiness of the left hand and fingers gradually occurred. Magnetic resonance imaging (MRI) of the left elbow revealed a swollen ulnar nerve with perineural enhancement involving anconeus epitrochlearis (AE) muscle within the cubital tunnel. The operation revealed adhesion of the AE muscle to the left ulnar nerve. Open in-situ decompression of the ulnar nerve without transposition eventually alleviated the pain and weakness associated with ulnar neuropathy. The patient slowly recovered 6 months after surgery. The AE muscle is a common anatomic variation, with a prevalence of up to 34%. However, the prevalence of ulnar neuropathy associated with the AE muscle is unknown. It is a congenital accessory muscle between the medial humeral epicondyle and the olecranon covering the posterior aspect of the cubital tunnel. It is usually diagnosed intraoperatively and not preoperatively in the absence of no imaging studies. The clinical presentation of ulnar neuropathy caused by the AE usually differs from idiopathic disease, including younger age at onset, rapid progression with a short duration of symptoms, and edema of the AE muscle on the MRI.

INTRODUCTION

Ulnar neuropathy involving the cubital tunnel is the second most common entrapment neuropathy, following carpal tunnel syndrome1. A number of risk factors for the development of cubital tunnel syndrome have been suggested, including diabetes mellitus, valgus or varus deformity of the elbow, repetitive tasks that require protracted elbow flexion, and the repetitive use of vibrating tools13. Anconeus epitrochlearis (AE) muscle is a congenital accessory muscle, which originates in the medial epicondyle (ME) of the humerus and inserts onto the olecranon (OL) process the ulna. It can be found in normal elbows with an incidence ranging between 4% to 34%7,11. AE is a common variation in the cubital tunnel retinaculum of the elbow; however, its association with ulnar neuropathy is rare.

CASE REPORT

A 24-year-old right-handed male patient presented with a 1-month history of numbness and weakness in his left hand and fingers (Figure 1A). Initially, a vague discomfort developed in his left medial elbow and left hypothenar and the fourth and fifth fingers without any precipitating event, followed by severe pain that occurred in the left medial elbow and hypothenar area 4th and 5th fingers. The pain was marked by severe swelling and aching, associated with numbness and hypersensitivity. For several days, pain also radiated to the left medial scapular area. During the first week of symptom onset, the severe pain prevented his left hand and arm completely. The pain interfered with sleep. The patient’s initial treatment included painkillers obtained from a pharmacy, followed by a visit to nearby hospitals; however, no specific diagnosis was established. The patient’s severe pain persisted. The finger movement became clumsy, which was misinterpreted suggesting that the hand and fingers could not be used due to severe pain in the medial hand and fingers. ing (MRI) findings ere the patient was referred for further evaluation.

Figure 1

Pain distribution and magnetic resonance imaging (MRI) findings of cubital tunnel syndrome associated with anconeus epitrochlearis (AE). Ⓐ: Pain distribution. Black area denotes the painful area with paresthesia and allodynia. Ⓑ: Sagittal (left) and coronal (right) T2-weighted images of the left elbow showing the ulnar nerve (arrowheads) compression by AE (arrows), with increased signal intensity of the nerve, suggesting intraneural edema. Ⓒ: Axial fat-suppression T2-weighted MRI (left) reveals compression of the swollen ulnar nerve (arrowhead) by the AE (arrow). Ⓓ: Enhanced, axial T1-weighted images of the lesion immediately distal to the cubital tunnel. Mild perineural enhancement was observed in the surrounding flexor carpi ulnaris muscle. ME: medial epicondyle; OL: olecranon.

Neurologic examination revealed the moderate weakness of the flexor digitorum profundus in the fourth and fifth fingers (grade 3/5). Abduction and adduction of the fingers were weak, which prevented any attempt to cross the middle finger over the index finger. Both Froment’s and Wartenber’s signs were positive. His sensations to light touch and pinprick were decreased in the left hypothenar area and the little and ulnar aspects of the ring finger. Mild allodynia to light touch was observed in the painful area. No pain (spontaneously or evoked) was elicited by passive movement of the elbow joint. No Tinel’s sign or tenderness overlying the ulnar nerve was detected in the cubital tunnel. The patient complained of persistent tingling paresthesia involving the medial wrist, hand, and little finger.

The electrophysiological study performed at the hospital where he was previously treated revealed acute ulnar neuropathy around the left elbow without mention of denervation. Because clinical and electrophysiological findings were consistent with acute ulnar neuropathy at the elbow with advanced motor signs, an MRI of the elbow was requested. MRI of the left elbow revealed diffuse swelling of the left ulnar nerve at and distal to the cubital canal (Figure 1B–D). The left ulnar nerve was compressed against ME by the AE muscle at the level of the cubital tunnel. Mild perineural enhancement of the left ulnar nerve just distal to the cubital tunnel was observed (Figure 1C, D). Laboratory parameters including erythrocyte sedimentation rate, C-reactive protein, rheumatoid factor, antinuclear antibody, and creatinine kinase were normal. Considering the course of ulnar nerve palsy and abnormal MRI findings, an exploration of the ulnar nerve was performed.

During the surgery, the fibrous facial layer (Osborne’s ligaments) over the cubital tunnel was not thickened or hypertrophied. The ulnar nerve was swollen with a slightly rubbery consistency (Figure 2A). The adhesion between the ulnar nerve and AE muscle was found and dissected (Figure 2B). The AE was excised and the ulnar nerve was distally dissected along its course to the flexor carpi ulnaris muscle. Although postoperative course was uneventful, the rate of recovery from ulnar neuropathy was not as fast as expected. The pinch and grip strength of the left hand and fingers did not show any improvement despite improvement in paresthesia until two months postoperatively. Then, the pinch and grip strength was gradually recovered with minimal paresthesia in the fifth finger and hypothenar area at 6 months postoperatively. No evidence of ulnar neuropathy was detected at 12 months postoperatively.

Figure 2

Intraoperative findings during decompression of the left cubital tunnel. Ⓐ: The left ulnar nerve (arrowhead) is compressed by the anconeus epitrochlearis (AE) muscle (arrows) within the Osborne’s ligament. Ⓑ: The left ulnar nerve (arrowhead) is decompressed following resection of the Osborne’s ligament and the AE muscle (arrows). MABC: medial antebrachial cutaneous nerve; ME: medial epicondyle.

DISCUSSION

1. AE Muscle

AE is a small triangular muscle originating in the ME of the humerus, inserting laterally on the OL and proximal posterior surface of the ulnar12. Its anatomic course is similar to that of the cubital tunnel retinaculum. It was postulated that the cubital tunnel retinaculum is the remnant of the AE muscle7. It expands and initiates the extension of the elbow and is regarded as a continuation of the triceps brachii muscle and enables extension of the forearm7. Thus, AE protects the ulnar nerve and assists the triceps muscle in preventing subluxation of the ulnar nerve. In contrast to the triceps, this muscle is innervated by a branch of the ulnar nerve9,11. The AE, when present, forms the roof of the cubital tunnel, replacing Osborne’s ligament13. It was suggested that Osborne’s ligament is a fibrous remnant of the AE that remains after the muscle regresses5. The anconeus muscle occupies more space than the typically present Osborne fascia6. The prevalence of this anomalous muscle is estimated to be 3% to 34% based on cadaveric and imaging studies and is often found bilaterally6,7,9,11.

2. AE and Cubital Tunnel Syndrome

The AE muscle exerts a compressive force on the ulnar nerve and its association with cubital tunnel syndrome has long been reported9,11. Although the AE is a common anatomical variation of the elbow, the prevalence of cubital tunnel syndrome due to AE is unknown4,9. Its association with cubital tunnel syndrome is generally detected during operation, not preoperatively4. It was suggested that ulnar neuropathy associated with AE might be dynamic rather than static compression and exhibited different clinical characteristics compared with idiopathic cubital tunnel syndrome including more rapid progression, younger age at onset, and shorter duration of symptoms2,4,9.

The current case also appeared as a sudden outbreak in young patients, as previously reported. The neurophysiological findings of ulnar neuropathy associated with AE also differ from those involving patients with idiopathic cubital tunnel syndrome2,3. Velocity drop or conduction block of the ulnar nerve indicating the subacute onset of symptoms is common rather than chronic demyelination generally seen in idiopathic ulnar neuropathy2,3.

Ultrasound and MRI are reliable imaging modalities used to show structural abnormalities of the cubital tunnel and can reveal the causes of secondary ulnar neuropathy and anatomical variants, as in the current patient. Edema of the AE in the MRI was associated with medial elbow pain8. In the MRI of the present case, the AE size was not large enough to directly compress the ulnar nerve, but close adhesion with the nerve was suspected (Figure 1). The adhesions between the AE and the ulnar nerve were confirmed by surgical findings (Figure 2). The ulnar nerve was swollen. A weak perineural enhancement of the ulnar nerve and flexor carpi ulnaris muscle was observed in the distal cubital tunnel. However, it is not known exactly whether this perineural enhancement is pathognomonic for ulnar neuropathy triggered by AE.

3. Treatment of Ulnar Neuropathy Associated with AE

Complete excision of the AE is widely accepted as the definitive treatment for the ulnar neuropathy associated with AE, but whether to transpose the ulnar nerve remains controversial10. Several treatment options have been suggested including muscular release or complete excision with in-situ decompression of the ulnar nerve and complete excision of the muscle with transposition of the ulnar nerve to prevent subluxation4, depending on the surgeon’s decision about the extent of neurolysis to prevent dislocation of the ulnar nerve and the extent of muscle excision. More rapid and complete recovery with a low incidence of recurrence than idiopathic cubital tunnel syndrome is a common finding in most studies investigating the AE muscle4,811,13. However, in the current case, the recovery was not prompt as reported in prior cases. The first sign of improvement was not observed until two months postoperatively. Based on our single case study, it is difficult to explain the delayed recovery.

Although excision of the AE in patients with cubital tunnel syndrome has been accepted as the definitive treatment, it was suggested that the AE prevents the development of cubital tunnel syndrome13). Wilson et al.13 reported a 5.4% prevalence of AE in patients with symptomatic cubital tunnel syndrome in their retrospective cohort study. It was significantly less than the reported prevalence (15.5%) of AE in asymptomatic patients13. Another retrospective cohort study by Maslow et al.9 reported similar results. The overall institutional prevalence of AE was 13.6% compared with a prevalence of 4.5% in operative patients with cubital tunnel syndrome9. It was suggested that AE is less rigid than the more common fascial layer of Osborne and may provide a more forgiving roof to the cubital tunnel and actually be more protective against the development of cubital tunnel syndrome13. Therefore, cubital tunnel syndrome is associated with AE when the muscle is hypertrophied or edematous13. Prior case reports hypothesized that ulnar neuropathy associated with AE may involve dynamic compression within the cubital tunnel because it is a muscular structure4. A more comprehensive study investigating the pathophysiology of cubital tunnel syndrome caused by AE is warranted in the near future.

CONCLUSION

The manifestations of ulnar neuropathy associated with AE differ from those of idiopathic cubital tunnel syndrome. They include younger age at onset, more rapid progression with a shorter duration of symptoms, neurophysiologic findings of velocity drop or conduction block of the ulnar nerve, and perineuritis and edema of AE on MRI. Therefore, when ulnar neuropathy due to cubital tunnel syndrome is suspected in young patients with rapid progression, an imaging study is essential to identify the structural lesion around the cubital tunnel.

Notes

No potential conflict of interest relevant to this article was reported.

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Figure 1

Pain distribution and magnetic resonance imaging (MRI) findings of cubital tunnel syndrome associated with anconeus epitrochlearis (AE). Ⓐ: Pain distribution. Black area denotes the painful area with paresthesia and allodynia. Ⓑ: Sagittal (left) and coronal (right) T2-weighted images of the left elbow showing the ulnar nerve (arrowheads) compression by AE (arrows), with increased signal intensity of the nerve, suggesting intraneural edema. Ⓒ: Axial fat-suppression T2-weighted MRI (left) reveals compression of the swollen ulnar nerve (arrowhead) by the AE (arrow). Ⓓ: Enhanced, axial T1-weighted images of the lesion immediately distal to the cubital tunnel. Mild perineural enhancement was observed in the surrounding flexor carpi ulnaris muscle. ME: medial epicondyle; OL: olecranon.

Figure 2

Intraoperative findings during decompression of the left cubital tunnel. Ⓐ: The left ulnar nerve (arrowhead) is compressed by the anconeus epitrochlearis (AE) muscle (arrows) within the Osborne’s ligament. Ⓑ: The left ulnar nerve (arrowhead) is decompressed following resection of the Osborne’s ligament and the AE muscle (arrows). MABC: medial antebrachial cutaneous nerve; ME: medial epicondyle.