Overview
Based on the records of traditional Chinese medicine, CBS has the functions of purifying the heart, eliminating phlegm, stimulating bile secretion, and soothing the nerves. It has the ability to alleviate fever, coma, delirium, epilepsy, convulsions in youngsters, dental caries, throat swelling, mouth ulcers, carbuncle, and furuncle.
Encephalitis is a neurological condition characterized by widespread or multiple inflammation of brain tissue. The causes of encephalitis are many and can stem from infectious organisms or be induced by autoimmune reactions, the latter being referred to as autoimmune encephalitis (AE). The yearly occurrence rate of encephalitis is 12.6 per 100,000 individuals. Among these cases, approximately 40-50% are caused by infectious factors, whereas 20-30% are attributed to autoimmune encephalitis (AE). The development of viral encephalitis involves the direct invasion of brain tissue by the virus and the immune response of the body to viral antigens. The virus multiplies extensively, leading to the degeneration of neurons, necrosis, the proliferation of glial cells, and the infiltration of inflammatory cells. These severe tissue reactions can result in the formation of demyelinating lesions and damage to blood vessels and the areas surrounding them. Additionally, vascular lesions affect the circulation in the brain and worsen the damage to brain tissue. The development of AE involves several factors, including molecular mimicry, the activation of latent antigen epitopes, the spread of antigen epitopes, and the disruption of the innate immune system caused by persistent pathogen infection.
The mechanisms that are clearer can be summarized as follows: (1) Decrease in the number of receptors on the surface due to cross-linking and internalization: Anti-NMDAR antibodies have the ability to attach to NMDAR on the postsynaptic membrane, resulting in a reduction of NMDAR surface density through cross-linking and internalization. This reduction leads to a decrease in NMDAR-mediated current, which in turn causes learning and memory defects. (2) Protein-protein interaction disruption: Anti-LGI1 antibodies can disrupt the binding between LGI1 and ADAM23 on the presynaptic membrane and ADAM22 on the postsynaptic membrane. This disruption leads to a decrease in the density of anti-α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor (AMPAR).
According to the aforementioned background processes, along with the most recent research, there was a decrease in the abundance of gut flora in patients with AE. Transplanting the fecal bacteria of individuals with anti-NMDAR encephalitis into mice's intestines resulted in cognitive impairment in the animals. This indicates that the brain-gut axis may have a significant role in the development of anti-NMDAR encephalitis. From a clinical perspective, patients consume CBS orally in order to achieve its therapeutic benefits. The primary constituents, bilirubin and bile acid, have been documented to possess regulatory effects on the gut microbiota. Thus, we hypothesize that CBS is probable to have neuroprotective and anti-inflammatory impacts on the brain through alterations in the intestinal microbiota and regulation of the brain-gut connection. CBS is expected to decrease the occurrence of symptomatic seizures and enhance the patient's level of consciousness and cognitive abilities.
Eligibility
Inclusion Criteria:
- Subjects must meet the following eligibility criteria at screening to participate in this study.
1.1 Inclusion criteria for subjects with autoimmune encephalitis (hereinafter referred to as AE) of all subtypes 1.1.1 Subjects are able to understand the purpose and risks of the study, provide informed consent, and authorize the use of confidential health information in accordance with national and local privacy regulations.
1.1.2. Tumors or malignancies can be reasonably excluded before the baseline visit (randomization), and screening guidelines for thymoma, teratoma, and malignant tumors should be followed.
1.1.3. Both men and women are welcome, and the age at the time of providing informed consent is 18-80 years old (inclusive).
1.1.4. Meet the diagnosis of AE (according to the Chinese Autoimmune Encephalitis Diagnosis and Treatment Expert Consensus 2022 Edition): A. Clinical manifestations: acute or subacute onset (<3 months), with one or more of the following neurological and psychiatric symptoms or clinical syndromes.
- a. Limbic system symptoms: recent memory loss, epileptic seizures, mental and behavioral abnormalities, one or more of the three symptoms.
- b. Encephalitis syndrome: clinical manifestations of diffuse or multifocal brain damage.
- c. Clinical manifestations of involvement of the basal ganglia and/or diencephalon/hypothalamus.
- d. Mental disorder, and the psychiatric specialist believes that it does not meet the non-organic disease.B. Auxiliary examination: one or more of the following auxiliary examination findings, or combined with related tumors.
- a. Abnormal cerebrospinal fluid: cerebrospinal fluid leukocytosis (>5×106/L), or cerebrospinal fluid cytology shows lymphocytic inflammation, or specific oligoclonal bands are positive.
- b. Neuroimaging or electrophysiological abnormalities: MRI limbic system T2 or FLAIR abnormal signals, unilateral or bilateral, or other areas of T2 or FLAIR abnormal signals (excluding nonspecific white matter changes and stroke); or PET imaging limbic system hypermetabolism changes, or multiple cortical and/or basal ganglia hypermetabolism. Figure 1 shows the typical neuroimaging manifestations of AE patients. Abnormal electroencephalogram, manifested as focal epilepsy or epileptiform discharge (located in the temporal lobe or outside the temporal lobe), or diffuse or multifocal slow wave rhythm. In adult patients with anti-NMDAR encephalitis, abnormal delta brush waves (extreme delta brush) often correspond to prolonged hospitalization and poor prognosis.
- c. Specific types of tumors associated with AE, such as limbic encephalitis combined with small cell lung cancer, anti-NMDAR encephalitis combined with ovarian teratoma.C. Confirmatory experiments: positive anti-neuronal antibodies. Including NMDA-R, LGI-1, CASPR2, IgLON5, GABAA/BR, GlyR, AMPAR and axonal protein-3α and intracellular substance antibodies anti-Hu, anti-Ma2, anti-CRMP5, anti-Yo, anti-double carrier protein, anti-GAD, etc.D. Reasonably exclude other causes (refer to the differential diagnosis section of the consensus).
Diagnostic criteria: including possible AEs and confirmed AEs:
- Possible AEs: meet the three diagnostic criteria of A, B and D.
- Confirmed AEs: meet the four diagnostic criteria of A, B, C and D. 1.1.5. AE
symptoms occurred ≤9 months before randomization 1.1.6. Subjects meet new AEs
- New onset: defined as subjects with NMDA-R or LGI-1 AEs and meeting the following
- criteria
-
- The mRS score measured at baseline is stable (at least 24 hours) and is ≥2 points.
- Received the first acute first-line treatment within 6 weeks before randomization (baseline visit).
- New onset: defined as subjects with NMDA-R or LGI-1 AEs and meeting the following
1.1.7. All females of childbearing potential and all males must use contraception
during the study and for at least 30 days after the last dose of study treatment. In
addition, subjects should not donate sperm or eggs during the study and for at least
30 days after the last dose of study treatment.
1.1.8. Stable neurological examination within 30 days before baseline (Visit 1).
1.2 Additional inclusion criteria for the NMDA-R AE cohort
In addition to the criteria outlined in Section 1.1, only subjects who met all of
the following criteria were eligible for inclusion in the NMDA-R AE cohort:
- Age ≥ 18 years at the time of informed consent
- Informed consent, as appropriate based on patient age, specific site, and
national criteria
- Suspected or definite NMDAR AE diagnosis as follows:
1.2.1. Suspected NMDAR encephalitis was diagnosed when all three of the following
criteria were met: 1.2.1.1 Rapid onset (less than 3 months) of at least four of the
following six cardinal symptoms:
- Abnormal (psychiatric) behavior or cognitive dysfunction
- Speech dysfunction (rushing speech, hypospeech, mutism)
- Seizures
- Ataxia, dyskinesia, or rigid/abnormal posture
- Decreased level of consciousness
- Autonomic dysfunction or central hypoventilation 1.2.1.2. At least one of the
following laboratory results:
- Abnormal EEG (focal or diffuse slow or disorganized activity, epileptic
activity, or extreme delta brushes)
- CSF with pleocytosis or oligoclonal bands 1.2.1.3. Reasonable exclusion of
other etiologies and other clear encephalitis syndromes: for example,
Bickerstaff brainstem encephalitis, acute disseminated encephalomyelitis,
Hashimoto encephalopathy, primary angiitis of the central nervous system (CNS),
Rasmussen encephalitis.
Note: If the above three groups of symptoms in criterion 1.2.1.1 are present and
accompanied by systemic teratoma, suspected NMDAR encephalitis can also be
diagnosed.
1.2.2 Definite NMDAR encephalitis can be diagnosed when the following three criteria
are met at the same time: 1.2.2.1. The presence of one or more of the six main
symptoms described in criterion 1.2.1.1 for suspected NMDAR encephalitis.
1.2.2.2. History of anti-NMDAR (GluN1) IgG antibodies detected in CSF using a
cell-based assay.
1.2.3. Reasonable exclusion of other etiologies and other well-defined encephalitis
syndromes: e.g., Bickerstaff brainstem encephalitis, acute disseminated
encephalomyelitis, Hashimoto encephalopathy, primary angiitis of the central nervous
system (CNS), Rasmussen encephalitis.
1.3 Other inclusion criteria for the LGI-1 AE cohort
In addition to the criteria outlined in Section 1.1, only subjects who meet all of
the following criteria are eligible for inclusion in the LGI1 AE cohort:
1.3.1 Age ≥ 18 years at the time of signing the informed consent For subjects who
are unable to provide informed consent due to the severity of their illness, the
informed consent may be signed by their legally authorized representative at the
time of obtaining the subject's consent, according to local requirements.
1.3.2 Diagnosis of LGI-1 AE
The diagnosis of LGI-1 encephalitis can be made when both of the following criteria
are met:
1.3.2.1 Documented history of anti-LGI-1 IgG antibodies (in serum or CSF) using a
cell-based assay.
1.3.2.2 Subacute onset (less than 4 months of development) of working memory
deficits, seizures (including faciobrachial dystonic seizures), or psychiatric
symptoms suggestive of limbic system involvement.
1.3.2.3 Diagnosis of LGI1 AE is reasonable when other etiologies and other
well-defined encephalitis syndromes are excluded: e.g., Bickerstaff brainstem
encephalitis, acute disseminated encephalomyelitis, Hashimoto encephalopathy,
primary CNS vasculitis, Rasmussen encephalitis.
1.4 Other inclusion criteria for the AA AE cohort
In addition to the criteria outlined in Section 1.1, only subjects who meet all of
the following criteria are eligible for inclusion in the AA AE cohort:
- Aged ≥ 18 years at the time of signing the informed consent form For subjects
who are unable to provide informed consent due to the severity of their
illness, the informed consent form may be signed by their legally authorized
representative when the subject agrees, according to local requirements.
- Diagnosis of AA AE Meet the diagnosis of AE in 1.1, negative for anti-NMDA
antibodies and anti-LGI-1 antibodies, and positive for at least one of the
other anti-neuronal antibodies.
1.5 Inclusion criteria for viral encephalitis (hereinafter referred to as VE) cohort
The following four conditions must be met simultaneously for diagnosis of VE:
- Primary condition: altered mental status, including decreased level of
consciousness, drowsiness, or abnormal mental behavior lasting ≥24 h; or new
onset of epileptic seizure
- Secondary condition: fever ≥38 °C (before or within 72 h after onset), or new
focal manifestations of the nervous system, or cerebrospinal fluid leukocytes
≥5×10^6/L, or cerebrospinal fluid cytology showing lymphocytic inflammation, or
imaging showing brain parenchymal lesions consistent with encephalitis, or
abnormal electroencephalogram consistent with encephalitis
- Confirmatory laboratory test: positive cerebrospinal fluid viral nucleic acid
(polymerase chain reaction or metagenomic next-generation sequencing), or
positive cerebrospinal fluid and/or serum antiviral antibody IgM
- Reasonable exclusion of other causes
1.6 Healthy cohort:
- Age ≥ 18 years old when signing the informed consent form
- Healthy adult subjects without underlying diseases
- Exclusion Criteria:
- Any clinically significant cardiac, endocrine, hematologic, hepatic,
immune, infectious, metabolic, urologic, pulmonary, neurological,
dermatologic, psychiatric, and renal disease or other major medical
history that the investigator determines would preclude participation
in the clinical trial.
- Any untreated teratoma or thymoma at the baseline visit
(randomization)
- Other causes of symptoms, including central nervous system infection,
septic encephalopathy, metabolic encephalopathy, epileptic disorders,
mitochondrial disease, Klein-Levin syndrome, Creutzfeldt-Jakob
disease, rheumatic disease, Reyes syndrome, or inborn errors of
metabolism.
- History of herpes simplex encephalitis within the previous 24 weeks.
1.5. Any surgical procedure within 4 weeks prior to baseline, except
laparoscopic surgery or minor surgery (defined as surgery requiring
only local anesthesia or conscious sedation, i.e., surgery that does
not require general, neuraxial, or regional anesthesia and can be
performed on an outpatient basis; e.g., toenail surgery, mole
surgery, wisdom tooth extraction), excluding thymoma or teratoma
removal.
- Planned surgery during the study (except minor surgery).
- History of severe allergic or anaphylactic reactions, or any allergic
reaction that the investigator believes may be exacerbated by any
component of study treatment.
- Current or history of malignant disease, including solid tumors and
hematologic malignancies (except for basal cell carcinoma and
squamous cell carcinoma that have been completely resected and
considered cured for at least 12 months prior to Day -1). Subjects
with cancer remission for more than 5 years prior to baseline (Visit
1) may be included after discussion with the sponsor/sponsor
approval.
- A history of gastrointestinal surgery (except appendectomy or
cholecystectomy performed more than 6 months before screening),
irritable bowel syndrome, inflammatory bowel disease (Crohn's
disease, ulcerative colitis), or other clinically significant active
gastrointestinal diseases in the opinion of the investigator.
- A history of clinically significant recurrent or active
gastrointestinal symptoms (e.g., nausea, diarrhea, dyspepsia,
constipation) within 90 days before screening, including the need to
start symptomatic treatment (e.g., start medication for
gastroesophageal reflux disease) or a change in symptomatic treatment
within 90 days before screening (e.g., dose increase).
- A history of diverticulitis or concurrent severe gastrointestinal
(GI) abnormalities (e.g., symptomatic diverticular disease) because
the investigator believes that this may lead to an increased risk of
complications such as GI perforation.
- A history of blood donation (1 unit or more), plasma donation, or
platelet donation within 90 days before screening.
- Active suicidal ideation within 6 months before screening, or a
history of suicide attempt within 3 years before screening.
- Based on the investigator's judgment, there are serious diseases or
abnormalities in the clinical laboratory test results that prevent
the patient from completing the study or participating in the study
safely.
- Pregnant or lactating, or planning to become pregnant during the
study or within 3 months after the last dose of the study drug; women
of childbearing potential must have a negative serum pregnancy test
result at screening and a negative urine pregnancy test result before
the start of the study.
- The subject's mental or physical condition will hinder the evaluation
of efficacy and safety.
- Systolic blood pressure >150 mmHg or <90 mmHg after sitting still for
5 minutes or before dosing at screening. If out of range, it can be
measured again at screening and before dosing. If the repeated
measurement value is still out of range, the subject shall not
receive the drug.
- Subjects with second or third degree atrioventricular block or sick
sinus syndrome, poorly controlled atrial fibrillation, severe or
unstable angina, congestive heart failure, myocardial infarction, or
significant ECG abnormalities, including corrected QT interval >450
msec (male) or 470 msec (female), where corrected QT interval is
determined based on the Fridericia correction method, within 3 months
prior to the screening visit.
- Planned elective procedures or surgeries at any time after signing
the Informed Consent Form by follow-up visit.
- Any condition that affects the absorption of study treatment (e.g.,
gastrectomy).
- History of hypersensitivity to heparin or history of heparin-induced
thrombocytopenia.
- Subjects with abnormalities in medical history, physical examination,
ECG, or diagnostic laboratory tests that the investigator considers
to be clinically relevant.
- History of human immunodeficiency virus (HIV) or positive test
results at screening.
- Current infection with hepatitis C (defined as positive hepatitis C
virus (HCV) antibodies and detectable HCV RNA). Subjects with
positive HCV antibodies and HCV RNA below the limit of detection are
eligible to participate in the study.
- Current infection with hepatitis B (defined as positive HBsAg and/or
positive total anti-HBc).
- Chronic, recurrent, or severe infection (e.g., pneumonia, sepsis)
within 90 days prior to baseline (visit 1).
- History of tuberculosis (TB) diagnosis or positive latent TB test
result.
- Symptoms of bacterial, fungal, or viral infection (including upper
respiratory tract infection) within 28 days prior to baseline (visit
1). Subjects with localized fungal infection (e.g., candidiasis,
tinea) are eligible for rescreening after successful treatment of the
infection.
- Infection requiring hospitalization or IV anti-infective medication
within 4 weeks prior to baseline visit.
- Any live or live attenuated vaccine within 28 days prior to baseline
(visit 1) or planned during the study.
- Contraindications to all of the following salvage therapies:
rituximab, intravenous immunoglobulin, high-dose corticosteroids, or
IV cyclophosphamide.
- History of or receipt of the following treatments: Total lymphoid
irradiation, cladribine, T-cell or T Cell recipient vaccination,
total body irradiation, or total lymphoid irradiation at any time.
Stem cell transplantation at any time.
- Abnormal laboratory values determined by the investigator to be
clinically significant at Screening or Baseline (Visit 1).
- Any of the following blood test abnormalities at Screening: a. White
blood cell count < 3.0 × 10^3/µL. b. Absolute neutrophil count < 2.0
× 10^3/µL. c. Absolute lymphocyte count < 0.5 × 10^3/µL. d. Platelet
count < × 10 × 10^4/µL. e. glutamic-pyruvic transaminase, glutamic
oxaloacetic transaminase, or γ-glutamyl transpeptidase ≥ 3 x upper
limit of normal (ULN) or bilirubin > 2 x ULN. f. glomerular
filtration rate ≤ 60 mL/min/1.73 m2. g. Lymphocyte count < lower
limit of normal
- Any of the following urine test abnormalities at Screening: a.
β-2-microglobulin>0.3 μg/mL. b. Albumin/creatinine ratio>22.6
mg/mmol.
- Previous participation in this study.
- Blood donation (1 unit or more) within 90 days before screening,
plasma donation within 1 week before screening, and platelet donation
within 6 weeks before screening.
- History of alcohol or drug abuse in the past year (determined by the
investigator).
- Pregnant or lactating subjects, as well as subjects planning to
become pregnant or start breastfeeding at any time during the study
and within 30 days after completion of study treatment.
- Participating in a clinical trial or having participated in a
clinical trial within 90 days before screening.
- History of clinically significant suicidal thoughts or behaviors in
the past 12 months as assessed by Columbia-Suicide Severity Rating
Scale at screening.
- Unwilling or unable to comply with protocol requirements.
- The patient has obvious hearing or vision impairment, language
barriers, claustrophobia, etc., which makes the patient unable to
cooperate with the neuropsychological scale assessment and MRI
examination.
- The researcher or sponsor believes that there are other unknown
reasons that make the subject unsuitable for inclusion.