Terminal latency index in polyneuropathy with IgM paraproteinemia and anti‐MAG antibody

Cocito, Dario; Isoardo, G.; Ciaramitaro, P.; Migliaretti, Giuseppe; Pipieri, A.; Barbero, P.; Cucci, Angele; Durelli, Luca

doi:10.1002/mus.1145

Cited by 62 publications

(49 citation statements)

References 22 publications

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“…2,5,6,11,19 Median TLI alone was sufficient to distinguish between MAG/SGPG-N and HMSN1 with a high specificity and moderately high sensitivity. Patients with median nerve TLI Ͻ0.26 had MAG/SGPG-N and those with TLI Ͼ0.32 had HMSN1.…”

Section: Discussionmentioning

confidence: 94%

“…2,5,6,29 A direct comparison of our data with those TLI values is difficult since it is influenced by the distal distance, which varied in different studies. Ulnar TLI was additionally evaluated in one study to increase the specificity in distinguishing MAG/SGPG-N from CIDP, 2,6 but in our study the combination of median and ulnar TLI did not appreciably improve classification into MAG/ SGPG-N or HMSN1.…”

Section: Discussionmentioning

confidence: 95%

“…2,5,29 TLI was shown to be significantly lower in patients with anti-MAG neuropathy than in those with CIDP. 6 In the upper extremity, TLI allows comparative assessment of the conduction time along the distal (wrist-to-thenar) nerve segment with that of the intermediate segment (elbow-to-wrist). MFR compares the conduction time along the distal segment of a nerve with its proximal one (spinal cord-to-elbow).…”

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confidence: 99%

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Terminal latency index in neuropathy with antibodies against myelin‐associated glycoproteins

et al. 2007

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Neuropathy with antibodies against myelin-associated glycoproteins (MAG/SGPG-N) and hereditary sensorimotor neuropathy type 1 (HMSN1) are characterized by chronic demyelination with little conduction block. Electrodiagnostic studies suggest that in HMSN1 conduction slowing occurs uniformly along the nerve, whereas in MAG/SGPG-N it is predominantly distal. Some but not all previous reports have shown that the terminal latency index (TLI) was useful to distinguish MAG/SGPG-N from chronic idiopathic demyelinating polyneuropathy. We compared median TLI from 21 patients with MAG/SGPG-N with those obtained from 26 patients with HMSN1, 20 with HMSN2, and 12 healthy volunteers. All patients with TLI <0.26 had MAG/SGPG-N, and all patients with TLI > or =0.32 had HMSN1. In the remaining patients with intermediate TLI values, ulnar distal motor latency (DML) aided in differentiation between MAG/SGPG-N and HMSN1 with an overall sensitivity of 100% and specificity of 98%. In conclusion, median TLI in combination with ulnar DML can further guide the demyelinating neuropathy evaluation toward hereditary or autoimmune causes.

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Section: Discussionmentioning

confidence: 94%

Section: Discussionmentioning

confidence: 95%

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confidence: 99%

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Terminal latency index in neuropathy with antibodies against myelin‐associated glycoproteins

et al. 2007

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“…In our patient, the TLIs of both peroneal nerves (0.62 and 0.60), both tibial nerves (0.63 and 0.58) and the right ulnar nerve (0.47) were greater than the mean values, as previously reported, although those of both median nerves (0.28 and 0.29) and the left ulnar nerve (0.38) were not greater than previously reported values. Cocito et al (12) measured TLIs in typical CIDP patients, as follows: 0.34-0.40 (median), 0.41-0.47 (ulnar), 0.34-0.38 (peroneal) and 0.40-0.48 (tibial). Compared to the values observed in these CIDP patients, the TLIs of our patient were also much higher in the lower extremities.…”

Section: Discussionmentioning

confidence: 99%

POEMS Syndrome Presenting with Acute Demyelinating Polyneuropathy: Increased Terminal Latency Indices and Uniform Demyelination

et al. 2013

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We herein report a case of polyneuropathy, organomegaly, endocrinopathy, M-protein and skin changes (POEMS) syndrome presenting with acute Guillain-Barré syndrome (GBS)-like features. The patient was healthy, except for mild dilated cardiomyopathy. She was unable to walk within ten days of the onset of weakness. A nerve conduction study (NCS) showed length-dependent, symmetric and non-focal demyelinating features with increased terminal latency indices (TLIs) in the lower limbs. Following the administration of intravenous immunoglobulin infusion, the proximal weakness of the lower extremities improved; however, the pleural effusion was aggravated and ascites newly developed. On further work-ups, splenomegaly, Mprotein and sclerotic bone changes were observed. This case suggests that, although rare, POEMS syndrome can present with acute demyelinating polyneuropathy resembling GBS and that characteristic NCS features such as increased TLI and uniform demyelination are helpful for the early diagnosis of POEMS syndrome.

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“…Die therapeutisch zu erzielende Verbesserung scheint aber bei Diabetes-Patienten geringer zu sein als bei CIDP-Patienten ohne Diabetes [24,13], was möglicherweise die vorbestehende Schädigung aufgrund einer latenten oder manifesten diabetischen Neuropathie widerspiegelt. [14] schlagen vor, dass die distale motorische Latenz, berechnet als "terminal latency index TLI" (distale Leitungsdistanz [mm]/Nervenleitgeschwindigkeit [m/s]×distal motorische Latenz [ms]), sensitiv die CIDP bei IgM-Paraproteinämie von anderen Formen des CIDP differenziert. Der reduzierte TLI ist auch zusammen mit einer verminderten sensiblen Nervenleitgeschwindigkeit bei normaler oder gering reduzierter motorischer Nervenleitgeschwindigkeit differenzialdiagnostisch hinweisend auf eine hereditäre Neuropathie mit Neigung zu Druckläsionen (HNPP, [3]).…”

Section: Hereditäre Neuropathienunclassified

Chronic inflammatory demyelinating polyneuropathy

et al. 2003

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Chronic inflammatory demyelinating polyneuropathy (CIDP) is an acquired immune-mediated disease of the peripheral nervous system with a prevalence of 1-2/100,000. Clinical and experimental findings suggest a role of immune pathomechanisms;however, the target antigens are still unknown. Beside classic CIDP with symmetrical proximal and distal paresis, subgroups of CIDP with pure motor or sensory deficits have been described. Diagnostic criteria include evidence of demyelination in electrophysiological examination and biopsy as well as elevated protein content in the CSF. Magnetic resonance imaging of plexuses and roots extends the diagnostic armamentarium and may be helpful in differential diagnosis. The utility of immunosuppressant/immunomodulatory therapies has been demonstrated in several studies.

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Terminal latency index in polyneuropathy with IgM paraproteinemia and anti‐MAG antibody

Cited by 62 publications

References 22 publications

Terminal latency index in neuropathy with antibodies against myelin‐associated glycoproteins

Terminal latency index in neuropathy with antibodies against myelin‐associated glycoproteins

POEMS Syndrome Presenting with Acute Demyelinating Polyneuropathy: Increased Terminal Latency Indices and Uniform Demyelination

Chronic inflammatory demyelinating polyneuropathy

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