| Literature DB >> 35049206 |
Abstract
RATIONALE: Guillain-Barré syndrome (GBS) is a postinfectious autoimmune peripheral neuropathy characterized by acute paralysis of the limbs. Clinically, extrahepatic manifestations of neurologic involvement in chronic hepatitis B (CHB) are uncommon. Little attention has been paid to the relationship between GBS and CHB viral infection. PATIENT CONCERNS: We presented a severe case of a 34-year-old man with general fatigue, anorexia, jaundice, numbness, and even muscle atrophy in the limbs, and respiratory failure during an acute exacerbation of CHB. DIAGNOSES: Serological liver enzymes test confirmed an acute exacerbation of CHB. Nerve conduction studies revealed the features of acute motor and sensory axonal neuropathy combined with acute inflammatory demyelinating polyneuropathy, and cerebrospinal fluid analysis showed albuminocytologic dissociation. Clinical manifestations and the test results were consistent with a diagnosis of severe CHB-related GBS.Entities:
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Year: 2021 PMID: 35049206 PMCID: PMC9191321 DOI: 10.1097/MD.0000000000027989
Source DB: PubMed Journal: Medicine (Baltimore) ISSN: 0025-7974 Impact factor: 1.817
Nerve conduction studies in the patient with CHB-related GBS.
| Latency (ms) | Amplitude∗ | Conduction velocity (m/s) | F-mean latency (ms) | ||||||
| Nerve | Stimulation site | RT | LT | RT | LT | RT | LT | RT | LT |
| Median (s) | Wrist – Digit II | NR | NR | NR | NR | NR | NR | ||
| Radial (s) | EPL tendon – Wrist | NR | NR | NR | NR | NR | NR | ||
| Ulnar (s) | Wrist – Digit V | 1.92 | 2.01 | 4.20† | 3.20† | 62.5 | 62.2 | ||
| Superficial peroneal (s) | Lower leg – Ankle | 2.07 | 2.03 | 7.60† | 9.60† | 43.5 | 49.3 | ||
| Sural (s) | Mid lower leg – Lat Malleolus | 2.01 | 1.90 | 8.30† | 12.0 | 49.8 | 42.1 | ||
| Median (m) | Wrist – APB | 4.37‡ | 4.29‡ | 0.46† | 0.25† | NR | NR | ||
| Elbow – Wrist | 9.72 | 8.99 | 0.12† | 0.10† | 51.4 | 56.4 | |||
| Ulnar (m) | Wrist – ADM | 2.38 | 2.63 | 4.80† | 4.20† | 31.40‡ | 31.30‡ | ||
| Bl. elbow – Wrist | 7.04 | 7.15 | 3.50† | 3.20† | 54.7 | 53.4 | |||
| Ab. elbow – Bl elbow | 8.79 | 9.06 | 2.20† | 2.70† | 54.3 | 52.4 | |||
| Peroneal (m) | Ankle – EDB | 4.84 | 5.08‡ | 0.16† | 0.96† | ||||
| Bl. Fib. head – Ankle | 14.0 | 12.40 | 0.13† | 0.59† | 40.4 | 47.8 | |||
| Tibial (m) | Ankle – Abd hal | 4.33 | 3.63 | 6.90 | 6.60 | 63.20‡ | 60.20‡ | ||
Figure 1Medical history and theragnostic course of a CHB-related GBS patient. CHB = chronic hepatitis B, GBS = Guillain–Barré syndrome, HBV = hepatitis B virus, IVIG = intravenous immunoglobulin, LP = lumbar puncture, NCS = nerve conduction studies, NICU = neurology intensive care unit.
Figure 2Muscle atrophy of the limbs. A: The obvious atrophy of dorsal interosseous muscles (arrow) in both hands. B and C: The obvious exposure of tibial anterior margin (arrow) in both lower legs.
Figure 3Liver function and MRC-sumscore during hospitalisation. ALT = alanine aminotransferase, AST = aspartate transaminase, MRC = Medical Research Council.
Clinical characteristics of CHB-related GBS.
| Virological markers | |||||||||
| Reference | Country or region | Age/sex | Duration of GBS onset from CHB | Symptoms | HBsAg | HBeAg | HBeAb | HBcAb | HBV-DNA |
| Tsukada et al (1987)[ | Japan | 34/M | 12 yr | Mo/Se/CP | + | − | + | + | NM |
| Japan | 48/F | NM | Mo/Se | + | NM | NM | NM | NM | |
| Han et al (1999)[ | Taiwan | 46/M | NM | Mo/Se | + | + | + | IgM (−) | NM |
| Taiwan | 29/M | 3 yr | Se | + | − | + | NM | + | |
| Chroni et al (2003)[ | Greece | 65/M | Ep 1: NM | Mo/Se/CP/RF | + | − | + | IgM (−), IgG (+) | 2235∗ |
| Ep 2: 4 yr | Mo/Se | NM | NM | NM | IgM (+) | 4∗ | |||
| Sonavane et al (2018)[ | India | 59/M | NM | Mo/CP | + | − | + | IgM (+) | 100,890† |
| Our case 2021 | Chinese mainland | 34/M | 2 yr | Mo/Se/MA/RF | + | − | + | IgM 1:502 | 110,000† |