Diagnosis
and Treatment Protocol for Novel Coronavirus Pneumonia
(Trial
Version 7)
(Released
by National Health Commission & State Administration of
Traditional
Chinese Medicine on March 3, 2020)
Since December 2019, multiple cases of novel coronavirus
pneumonia (NCP) have been identified in Wuhan, Hubei. With the spread of the
epidemic, such cases have also been found in other parts of China and other
countries. As an acute respiratory infectious disease, NCP has been included in
Class B infectious diseases prescribed in the Law of the People's Republic of
China on Prevention and Treatment of Infectious Diseases, and managed as an
infectious disease of Class A. By taking a series of preventive control and
medical treatment measures, the rise of the epidemic situation in China has
been contained to a certain extent, and the epidemic situation has eased in
most provinces, but the incidence abroad is on the rise. With increased
understanding of the clinical manifestations and pathology of the disease, and
the accumulation of experience in diagnosis and treatment, in order to further
strengthen the early diagnosis and early treatment of the disease, improve the
cure rate, reduce the mortality rate, avoid nosocomial infection as much
as possible and pay attention to the spread caused by the imported cases from
overseas, we revised the Diagnosis and
Treatment Protocol for Novel Coronavirus Pneumonia (Trial Version 6) to Diagnosis and Treatment Protocol for Novel
Coronavirus Pneumonia (Trial Version 7).
I. Etiological Characteristics
The novel coronaviruses belong to the β genus. They have envelopes,
and the particles are round or oval, often polymorphic, with diameter being 60
to 140 nm. Their genetic characteristics are significantly different from
SARS-CoV and MERS-CoV. Current research shows that they share more than 85%
homology with bat SARS-like coronaviruses (bat-SL-CoVZC45). When isolated and
cultured in vitro, the 2019-nCoV can be found in human respiratory epithelial
cells in about 96 hours, however it takes about 6 days for the virus to be
found if isolated and cultured in Vero E6 and Huh-7 cell lines.
Most of the knowledge about the physical and chemical
properties of coronavirus comes from the research on SARS-CoV and MERS-CoV. The
virus is sensitive to ultraviolet and heat. Exposure to 56°C for 30 minutes and
lipid solvents such as ether, 75% ethanol, chlorine-containing disinfectant,
peracetic acid, and chloroform can effectively inactivate the virus.
Chlorhexidine has not been effective in inactivating the virus.
II. Epidemiological Characteristics
1. Source
of infection
Currently, the patients infected by the novel coronavirus
are the main source of infection; asymptomatic infected people can also be an
infectious source.
2. Route
of transmission
Transmission
of the virus happens mainly through respiratory droplets and close contact.
There is the possibility of aerosol transmission in a relatively closed
environment for a long-time exposure to high concentrations of aerosol. As the
novel coronavirus can be isolated in feces and urine, attention should be paid
to feces or urine contaminated environment that may lead to aerosol or contact
transmission.
3. Susceptible
groups
People are generally susceptible.
III. Pathological changes
Pathological findings from limited autopsies and biopsy
studies are summarized below: 1. Lungs
Variable consolidation is present in the
lungs.
The alveoli are filled with fluid and fibrin with hyaline
membrane formation. Macrophages and many
multinucleated syncytial cells are identified within the alveolar exudates.
Type II pneumocytes show marked
hyperplasia and focal desquamation.
Viral inclusions are observed in type II pneumocytes and macrophages. In
addition, there is prominent edema and congestion in the alveolar septa which
are infiltrated by monocytes and lymphocytes.
Fibrin microthrombi are present.
In more severely affected area, hemorrhage, necrosis, and overt
hemorrhagic infarction are seen. Organization of alveolar exudates and
interstitial fibrosis are also present.
Detached epithelial cell and mucus are present in the
bronchi, sometimes mucus plugs are seen.
Hyperventilated alveoli, interrupted alveolar interstitium
and cystic formation are occasionally seen.
By electronic microscopy, cytoplasmic 2019-nCoV virions are
observed in the bronchial epithelium and type II pneumocytes. Immunostain
reveals 2019-nCoV viral immunoreactivity in some alveolar epithelial cells and
macrophages and RT-PCR confirms the presence of 2019-nCoV nucleic acid.
2.
Spleen, hilar lymph nodes and bone marrow
The spleen is markedly atrophic with a decreased number of
lymphocytes. Focal hemorrhage and
necrosis are present. Macrophages proliferation and phagocytosis are present in
the spleen. Sparsity of lymphocytes and focal necrosis are noted in lymph
nodes. CD4+ and CD8+ immunohistochemistry highlights a decreased number of T
cells in the spleen and lymph nodes. Myelopoiesis is decreased in bone marrow.
3.
Heart and blood vessels
Degenerated or necrosed myocardial cells are present, along
with mild infiltration of monocytes, lymphocytes and/or neutrophils in the
cardiac interstitium. Shedding of endothelial cells, endovasculitis and thrombi
are seen in some blood vessels.
4.
Liver and gall bladder
The liver is dark-red and enlarged. Degeneration and focal
necrosis of hepatocytes are found, accompanied by infiltration of neutrophils.
The sinusoids are congested. The portal areas are infiltrated by lymphocytes
and histiocytes. Microthrombi are seen. The gallbladder is prominently
distended.
5.
Kidneys
The kidneys are remarkable for proteinaceous exudates in
the Bowman’s capsule around glomeruli, degeneration and shedding of renal
tubules epithelial cells, and hyaline casts. Microthrombi and fibrotic foci are
found in the kidney interstitium.
6.
Other organs
Cerebral hyperemia and edema are present, with degeneration
of some neurons. Necrotic foci are noted in the adrenal glands. Degeneration,
necrosis and desquamation of epithelium mucosae of variable degree are present
in the esophageal, stomach and bowel.
IV. Clinical Characteristics
1. Clinical manifestations
Based on the current epidemiological investigation, the
incubation period is one to 14 days, mostly three to seven days.
The main manifestations include fever, fatigue and dry
cough. Nasal congestion, runny nose, sore throat, myalgia and diarrhea are
found in a few cases. Severe patients develop dyspnea and/or hypoxemia after
one week and may progress rapidly to acute respiratory distress syndrome,
septic shock, refractory metabolic acidosis, coagulopathy, multiple organ
failure etc. It is noteworthy that for severe and critically ill patients may
only present with moderate to low fever, or even no fever at all.
Some children and neonatal patients may have atypical
symptoms, presented with gastrointestinal symptoms such as vomiting and
diarrhea, or only manifested as lethargy and shortness of breath.
The patients with mild symptoms usually do not develop
pneumonia but have low fever and mild fatigue.
Based on our
experience, most patients have good prognosis and a small percentage of
patients are critically ill. The prognosis for the elderly and patients with
chronic underlying diseases is poorer. The clinical course of pregnant women
with NCP is similar to that of non-pregnant patients of the same age. Symptoms
in children are relatively mild. 
2. Laboratory tests
General findings
In the early stages of the disease, peripheral WBC count is
normal or decreased and the lymphocyte count is decreased. Some patients have
elevated liver enzymes, lactate dehydrogenase (LDH), muscle enzymes and
myoglobin. Elevated troponin is seen in some critically ill patients. Most
patients have elevated C-reactive protein and erythrocyte sedimentation rate
and normal procalcitonin. In severe cases, D-dimer increases and peripheral
blood lymphocytes progressively decrease. Severe and critically ill patients
often have elevated inflammatory factors.
Pathogenic and serological findings
(1)
Pathogenic findings: Novel coronavirus nucleic
acid can be detected in nasopharyngeal swabs, sputum, lower respiratory tract
secretions, blood, feces and other specimens using RT-PCR and/or NGS methods.
It is more accurate if specimens are obtained from lower respiratory tract
(sputum or air tract extraction). The specimens should be submitted for testing
as soon as possible after collection.
(2)
Serological findings: NCP virus specific IgM
becomes detectable around 3-5 days after onset; IgG reaches a titration of at
least 4-fold increase during convalescence compared with the acute phase.
3. Chest imaging
In the early stage, imaging shows multiple small patchy
shadows and interstitial changes, more apparent in the peripheral zone of
lungs. As the disease progresses, imaging shows multiple ground glass opacities
and infiltration in both lungs. In severe cases, pulmonary consolidation may
occur. However, pleural effusion is rare.
V. Case Definitions
1. Suspect cases
Considering both the following
epidemiological history and clinical manifestations:
1.1 Epidemiological history
1.1.1 History of
travel to or residence in Wuhan and its surrounding areas, or in other
communities where cases have been reported within 14 days prior to the onset of
the disease;
1.1.2 In contact with novel coronavirus infected people
(with positive results for the nucleic acid test) within 14 days prior to the
onset of the disease; 
1.1.3 In contact with patients who have fever or
respiratory symptoms from Wuhan and its surrounding area, or from communities
where confirmed cases have been reported within 14 days before the onset of the
disease; or
1.1.4 Clustered cases (2 or more cases with fever and/or
respiratory symptoms in a small area such families, offices, schools etc within
2 weeks).
1.2 Clinical manifestations 
1.2.1 Fever and/or respiratory symptoms;
1.2.2 The aforementioned imaging
characteristics of NCP;
1.2.3 Normal or decreased WBC count, normal or decreased
lymphocyte count in the early stage of onset. 
A suspect case has any of the epidemiological history plus
any two clinical manifestations or all three clinical manifestations if there
is no clear epidemiological history.
2. Confirmed cases
Suspect cases with one of the following
etiological or serological evidences:
2.1 Real-time fluorescent RT-PCR indicates
positive for new coronavirus nucleic acid;
2.2 Viral gene sequence is highly
homologous to known new coronaviruses.
2.3 NCP virus specific Ig M and IgG are detectable in
serum; NCP virus specific IgG is detectable or reaches a titration of at least
4-fold increase during convalescence compared with the acute phase.
VI. Clinical Classification
1.
Mild cases
The clinical symptoms were mild, and there
was no sign of pneumonia on imaging.
2.
Moderate cases
Showing fever and respiratory symptoms
with radiological findings of pneumonia.
3.
Severe cases
Adult cases meeting any of the following criteria:
(1) Respiratory
distress (≧30
breaths/ min);
(2) Oxygen
saturation≤93%
at rest;
(3) Arterial
partial pressure of oxygen (PaO2)/ fraction of inspired oxygen (FiO2)≦
300mmHg (l mmHg=0.133kPa).
In
high-altitude areas (at an altitude of over 1,000 meters above the sea level),
PaO2/ FiO2 shall be corrected by the following
formula:
PaO2/ FiO2 x[Atmospheric
pressure (mmHg)/760]
Cases with chest imaging that shows obvious lesion
progression within 24-48 hours >50% shall be managed as severe cases.
infants aged 2-12 months; RR ≥ 40 BPM for children aged 1-5
years, and RR ≥ 30 BPM for children above 5 years old) independent of fever and
crying;
(2) Oxygen
saturation ≤ 92% on finger pulse oximeter taken at rest;
(3) 
Labored breathing
(moaning, nasal fluttering, and infrasternal, supraclavicular and intercostal
retraction), cyanosis, and intermittent apnea;
Labored breathing
(moaning, nasal fluttering, and infrasternal, supraclavicular and intercostal
retraction), cyanosis, and intermittent apnea;
(4) Lethargy
and convulsion;
(5) Difficulty
feeding and signs of dehydration.
4.
Critical cases
Cases meeting any of the following
criteria:
4.1 Respiratory
failure and requiring mechanical ventilation;
4.2 Shock;
4.3 With
other organ failure that requires ICU care.
VII. Clinical early warning indicators of severe
and critical cases
1. Adults.
1.1 The
peripheral blood lymphocytes decrease progressively;
1.2 Peripheral
blood inflammatory factors, such as IL-6 and C-reactive proteins, increase
progressively;
1.3 Lactate
increases progressively;
1.4 Lung
lesions develop rapidly in a short period of time.
2. Children.
2.1 Respiratory
rate increased;
2.2 Poor
mental reaction and drowsiness;
2.3 Lactate
increases progressively;
2.4 Imaging
shows infiltration on both sides or multiple lobes, pleural effusion or
rapid progress of lesions in a short period of time;
2.5 Infants
under the age of 3 months who have either underlying diseases (congenital heart
disease, bronchopulmonary dysplasia, respiratory tract deformity, abnormal
hemoglobin, and severe malnutrition, etc.) or immune deficiency or hypofunction
(long-term use of immunosuppressants).
VIII.
Differential Diagnosis 
1.
The mild manifestations of NCP need to be
distinguished from those of upper respiratory tract infections caused by other
viruses.
2.
NCP is mainly distinguished from other known
viral pneumonia and mycoplasma pneumoniae infections
such as influenza virus, adenovirus and respiratory syncytial virus. For
suspect cases, efforts should be made to use methods such as rapid antigen
detection and multiplex PCR nucleic acid testing for detection of common
respiratory pathogens.
3.
NCP should also be distinguished from non-infectious
diseases such as vasculitis, dermatomyositis and organizing pneumonia.
IX. Case Finding and Reporting
Health professionals in medical institutions of all types
and at all levels, upon discovering suspect cases that meet the definition, should
immediately keep them in single room for isolation and treatment. If the cases
are still considered as suspected after consultation made by hospital experts
or attending physicians, it should be reported directly online within 2 hours;
samples should be collected for new coronavirus nucleic acid testing and
suspect cases should be safely transferred to the designated hospitals
immediately. People who have been in close contact with confirmed patients are
advised to perform new coronavirus pathogenic testing in a timely manner, even
though common respiratory pathogens are tested positive.
If two nucleic acid tests, taken at least 24-hour apart, of
an NCP suspect case are negative, and the NCP virus specific IgM and IgG are
negative after 7 days from onset, the suspect diagnosis can be ruled out.
X. Treatment
1.
Treatment venue determined by the severity of
the disease
1.1
Suspected and confirmed cases should be isolated
and treated at designated hospitals with effective isolation, protection and
prevention conditions in place. A suspect case should be treated in
isolation in a single room. Confirmed cases can be treated in the same room.
1.2
Critical cases should be admitted to ICU as soon
as possible.
2.
General treatment
2.1
Letting patients rest in bed and strengthening
support therapy; ensuring sufficient caloric intake for patients; monitoring
their water and electrolyte balance to maintain internal environment stability;
closely monitoring vital signs and oxygen saturation.
2.2
According to patients’ conditions, monitoring
blood routine result, urine routine result, c-reactive protein (CRP),
biochemical indicators (liver enzyme, myocardial enzyme, renal function etc.),
coagulation function, arterial blood gas analysis, chest imaging and
cytokines detection if necessary.
2.3
Timely providing effective oxygen therapy,
including nasal catheter and mask oxygenation and nasal high-flow oxygen therapy.
If possible, inhalation of mixed hydrogen and oxygen (H2/O2:
66.6%/33.3%) can be applied.
2.4
Antiviral
therapy: Hospitals can try Alpha-interferon (5 million U or equivalent dose
each time for adults, adding 2ml of sterilized water, atomization inhalation
twice daily), lopinavir/ritonavir (200 mg/50mg per pill for adults, two pills
each time, twice daily, no longer than 10 days), Ribavirin (suggested to be
used jointly with interferon or lopinavir/ritonavir, 500 mg each time for
adults, twice or three times of intravenous injection daily, no longer than 10
days), chloroquine phosphate (500 mg bid for 7 days for adults aged 18-65 with
body weight over 50 kg; 500 mg bid for Days 1&2 and 500 mg qd for Days 3-7
for adults with body weight below 50 kg), Arbidol (200 mg tid for adults, no
longer than 10 days). Be aware of the adverse reactions, contraindications (for
example, chloroquine cannot be used for patients with heart diseases) and
interactions of the abovementioned drugs. Further evaluate the efficacy of
those drugs currently being used. Using three or more antiviral drugs at the
same time is not recommend; if an intolerable toxic side effect occurs, the
respective drug should be discontinued. For the treatment of pregnant women,
issues such as the number of gestational weeks, choice of drugs having the
least impact on the fetus, as well as whether pregnancy being terminated before
treatment should be considered with patients being informed of these
considerations.
Antiviral
therapy: Hospitals can try Alpha-interferon (5 million U or equivalent dose
each time for adults, adding 2ml of sterilized water, atomization inhalation
twice daily), lopinavir/ritonavir (200 mg/50mg per pill for adults, two pills
each time, twice daily, no longer than 10 days), Ribavirin (suggested to be
used jointly with interferon or lopinavir/ritonavir, 500 mg each time for
adults, twice or three times of intravenous injection daily, no longer than 10
days), chloroquine phosphate (500 mg bid for 7 days for adults aged 18-65 with
body weight over 50 kg; 500 mg bid for Days 1&2 and 500 mg qd for Days 3-7
for adults with body weight below 50 kg), Arbidol (200 mg tid for adults, no
longer than 10 days). Be aware of the adverse reactions, contraindications (for
example, chloroquine cannot be used for patients with heart diseases) and
interactions of the abovementioned drugs. Further evaluate the efficacy of
those drugs currently being used. Using three or more antiviral drugs at the
same time is not recommend; if an intolerable toxic side effect occurs, the
respective drug should be discontinued. For the treatment of pregnant women,
issues such as the number of gestational weeks, choice of drugs having the
least impact on the fetus, as well as whether pregnancy being terminated before
treatment should be considered with patients being informed of these
considerations.
2.5
Antibiotic drug treatment: Blind or inappropriate
use of antibiotic drugs should be avoided, especially in combination with
broad-spectrum antibiotics.
3.
Treatment of severe and critical cases
3.1
Treatment principle: On the basis of symptomatic
treatment, complications should be proactively prevented, underlying diseases
should be treated, secondary infections also be prevented, and organ function
support should be provided timely.
3.2
Respiratory support:
3.2.1
Oxygen therapy: Patients with severe symptoms
should receive nasal cannulas or masks for oxygen inhalation and timely
assessment of respiratory distress and/or hypoxemia should be performed.
3.2.2
High-flow nasal-catheter oxygenation or
noninvasive mechanical ventilation: When respiratory distress and/or hypoxemia
of the patient cannot be alleviated after receiving standard oxygen therapy,
high-flow nasal cannula oxygen therapy or non-invasive ventilation can be
considered. If conditions do not improve or even get worse within a short time
(1-2 hours), tracheal intubation and invasive mechanical ventilation should be
used in a timely manner.
3.2.3
Invasive mechanical ventilation: Lung protective
ventilation strategy, namely low tidal volume (6-8ml/kg of ideal body weight)
and low level of airway platform pressure (<30cmH2O) should be
used to perform mechanical ventilation to reduce ventilator-related lung
injury. While the airway platform pressure maintained ≤30cmH2O, high PEEP can
be used to keep the airway warm and moist; avoid long sedation and wake the
patient early for lung rehabilitation. There are many cases of human-machine
asynchronization, therefore sedation and muscle relaxants should be used in a
timely manner. Use closed sputum suction according to the airway secretion, if
necessary, administer appropriate treatment based on bronchoscopy
findings.
3.2.4
Rescue therapy: Pulmonary re-tensioning is
recommended for patients with severe ARDS. With sufficient human resources,
prone position ventilation should be performed for more than 12 hours per day.
If the outcome of prone position ventilation is poor, extracorporeal membrane
oxygenation (ECMO) should be considered as soon as possible. Indications
include: ①When
Fi02>90%,
the oxygenation index is less than 80mmHg for more than 3-4 hours; ②For patients
with only respiratory failure when the airway platform pressure ≥ 35cmH2O, VV-ECMO
mode is preferred; if circulatory support is needed,
VAECMO mode should be used. When underlying diseases are under control and the
cardiopulmonary function shows signs of recovery, withdrawal of ECMO can be
tried.
3.3
Circulatory
support: On the basis of adequate fluid resuscitation, efforts should be made
to improve microcirculation, use vasoactive drugs, closely monitor changes in
blood pressure, heart rate and urine volume as well as lactate and base excess
in arterial blood gas analysis. If necessary, use non-invasive or invasive
hemodynamic monitor such as Doppler ultrasound, echocardiography, invasive
blood pressure or continuous cardiac output (PiCCO) monitoring. In the process
of treatment, pay attention to the liquid balance strategy to avoid excessive
or insufficient fluid intake.
Circulatory
support: On the basis of adequate fluid resuscitation, efforts should be made
to improve microcirculation, use vasoactive drugs, closely monitor changes in
blood pressure, heart rate and urine volume as well as lactate and base excess
in arterial blood gas analysis. If necessary, use non-invasive or invasive
hemodynamic monitor such as Doppler ultrasound, echocardiography, invasive
blood pressure or continuous cardiac output (PiCCO) monitoring. In the process
of treatment, pay attention to the liquid balance strategy to avoid excessive
or insufficient fluid intake.
If the heart rate suddenly increases more than 20% of the
basic value or the decrease
of blood pressure is more than 20% of the basic value with
manifestations of poor skin perfusion and decreased urine volume, make sure to
closely observe whether the patient has septic shock, gastrointestinal
hemorrhage or heart failure.
3.4
Renal failure and renal replacement
therapy: Active efforts should be made to look for causes for renal function
damage in critical cases such as low perfusion and drugs. For the treatment of
patients with renal failure, focus should be on the balance of body fluid, acid
and base and electrolyte balance, as well as on nutrition support including
nitrogen balance and the supplementation of energies and trace elements. For
critical cases, continuous renal replacement therapy (CRRT) can be used. The
indications include: ①
hyperkalemia; ②
acidosis; ③
pulmonary edema or water overload; ④ fluid management in multiple organ dysfunction.
3.5
Convalescent plasma treatment: It is suitable
for patients with rapid disease progression, severe and critically ill
patients. Usage and dosage should refer to Protocol
of Clinical Treatment with Convalescent Plasma for NCP Patients (2nd
trial version).
3.6
Blood purification treatment: Blood purification
system including plasma exchange, absorption, perfusion and blood/plasma
filtration can remove inflammatory factors and block "cytokine
storm", so as to reduce the damage of inflammatory reactions to the body.
It can be used for the treatment of severe and critical cases in the early and
middle stages of cytokine storm.
3.7
Immunotherapy:
For patients with extensive lung lesions and severe cases who also show an
increased level of IL-6 in laboratory testing, Tocilizumab can be used for
treatment. The initial dose is 4-8mg/kg with the recommended dose of 400mg
diluted with 0.9% normal saline to 100ml. The infusion time should be more than
1 hour. If the initial medication is not effective, one extra administration
can be given after 12 hours (same dose as before). No more than two
administrations should be given with the maximum single dose no more than
800mg. Watch out for allergic reactions. Administration is forbidden for people
with active infections such as tuberculosis.
Immunotherapy:
For patients with extensive lung lesions and severe cases who also show an
increased level of IL-6 in laboratory testing, Tocilizumab can be used for
treatment. The initial dose is 4-8mg/kg with the recommended dose of 400mg
diluted with 0.9% normal saline to 100ml. The infusion time should be more than
1 hour. If the initial medication is not effective, one extra administration
can be given after 12 hours (same dose as before). No more than two
administrations should be given with the maximum single dose no more than
800mg. Watch out for allergic reactions. Administration is forbidden for people
with active infections such as tuberculosis.
3.8
Other therapeutic measures
For patients with progressive deterioration of oxygenation
indicators, rapid progress in imaging and excessive activation of the body's
inflammatory response, glucocorticoids can be used in a short period of time
(three to five days). It is recommended that dose should not exceed the
equivalent of methylprednisolone 1-2 mg/kg/day. Note that a larger dose of
glucocorticoid will delay the removal of coronavirus due to immunosuppressive
effects. Xuebijing 100ml/time can be administered intravenously twice a day.
Intestinal microecological regulators can be used to maintain intestinal
microecological balance and prevent secondary bacterial infections.
Child severe and critical cases can be given
intravenous infusion of γ-globulin. For pregnant severe and critical cases, pregnancy
should be terminated preferably with csection.
Patients often suffer from anxiety and fear and they should
be supported by psychological counseling.
4.
Traditional Chinese Medicine treatment
This disease belongs to the category of plague in
traditional Chinese medicine (TCM), caused by the epidemic pathogenic factors.
According to the different local climate characteristic and individual state of
illness and physical conditions, the following treatment Protocol may vary. The
use of over-pharmacopoeia doses should be directed by a physician.
4.1
During medical observation
Clinical manifestation 1: fatigue and
gastrointestinal discomfort
Recommended Chinese patent medicine: Huoxiang Zhengqi
capsules (pills, liquid, or oral solution)
Clinical manifestation 2: fatigue and
fever
Recommended
Chinese patent medicine: Jinhua Qinggan granules, Lianhua Qingwen capsules
(granules), Shufeng Jiedu capsules (granules), Fangfeng Tongsheng pills
(granules)
4.2
During clinical treatment (confirmed cases)
4.2.1
Lung cleansing & detoxifying decoction
Scope
of application: It is suitable for light, moderate and severe patients, and can be used reasonably in
combination with the actual situation of patients in the treatment of
critically ill patients.
Recommended prescription: Ephedra 9g,
Zhigancao 6g, Almond 9g, Gypsum 15-30g
(fried
first), Guizhi 9g, Zixie 9g, Zhuling 9g, Baizhu 9g, Zhiling 15g, Bupleurum 16g,
Scutellaria baicalensis 6g, and Pinellia 9g , Ginger 9g, aster 9g, winter
flower 9g, shoot dry 9g, asarum 6g, yam 12g, coriander fruit 6g, tangerine peel
6g, aquilegia 9g. Suggested use: Traditional Chinese medicine decoction pieces
for decocting in water. One dose per day, twice in the morning and evening (forty
minutes after a meal), take with warm water, and three doses a course.
If
conditions permit, the patient can take half a bowl of rice soup each time
after taking the medicine, and can take
up to one bowl if the patient has a dry tongue and is deficient in bodily
fluids. (Note: If the patient does not have a fever, the amount of gypsum
should be little. If having a fever or strong heat, the amount of gypsum can be
increased). If the symptoms improve but do not fully recover, then take the
second course of treatment. If the patient has special conditions or other
underlying diseases, the prescription of the second course of treatment can be
modified based on the actual situation and the medicine should be discontinued
when the symptoms disappear.
Source of prescription: Notice on Recommending the Use of ‘Lung
cleansing & detoxifying decoction’ in Treatment of NCP by Integrated
Traditional Chinese and Western Medicine by the Office of the State
Administration of Traditional Chinese
Medicine & the General Office of the
National Health Commission. (2022 No.22)
4.2.2 Mild
cases
4.2.2.1 Cold dampness and stagnation lung
syndrome
Clinical manifestations: fever, fatigue, sore body, cough,
expectoration, chest tightness, suffocation, loss of appetite, nausea,
vomiting, sticky stools. Tongue has thin fat tooth mark or is faint red, and
the coating is white thick rot or white greasy and the pulse is moisten or
slippery.
Recommended
prescription: Raw ephedra 6g, raw gypsum 15g, almond 9g, loquat 15g, gardenia
15g, Guanzhong 9g, Dilong 15g, Xu Changqing 15g, Huoxiang 15g, Peilan 9g,
Cangzhu 15g, Yunling 45g, Atractylodes 30g, Jiao Sanxian 9g each , Magnolia
officinalis 15g, betel coconut 9g, yarrow fruit 9g, ginger 15g.
Suggested use: one dose daily, boiled with 600ml water,
take it three times at morning, noon and evening before meal. 
4.2.2.2 Dampness and heat-accumulation
lung syndrome
Clinical manifestations: low or no fever, slight chills,
fatigue, heavy head and body, muscle soreness, dry cough, low phlegm, sore
throat, dry mouth, do not want to drink more, or accompanied by chest
tightness, no sweat or sweating, Or vomiting and loss of appetite, diarrhea or
sticky stool. The tongue is reddish, and the coating is white, thick and greasy
or thin yellow, and the pulse is slippery or sloppy.
Recommended prescription: Betel nut 10g, apple 10g,
Magnolia 10g, Zhimu 10g, scutellaria baicalensis 10g, Bupleurum 10g, red peony
10g, forsythia 15g, artemisia annua 10g (decocted later), 10g of green leaves,
10g of green leaves, 5g of raw licorice. Suggested use: one dose daily, boiled with 400ml water, take it twice at morning
and evening.
4.2.3 Moderate cases
4.2.3.1 Dampness and stagnation lung
syndrome
Clinical manifestations: fever, low cough and sputum, or
yellow sputum, suffocation, shortness of breath, bloating, and constipation.
The tongue is dark red and fat; the coating is greasy or yellow and the pulse
is slippery or stringy.
Recommended prescription: raw ephedra 6g, bitter almond
15g, raw gypsum 30g, raw coix seed 30g, grass root 10g, patchouli 15g,
artemisia annua 12g, Polygonum cuspidatum 20g, verbena 30g, dried reed root
30g, gardenia 15g 15g of orange red, 10g of raw licorice. Suggested use: one
dose daily, boiled with 400ml water, take it twice at morning and evening.
4.2.3.2 Cold dampness lung syndrome
Clinical manifestations: low fever, low body temperature,
or no heat, dry cough, low sputum, fatigue, chest tightness, nausea, or nausea.
The tongue is pale or red, and the coating is white or greasy, and the veins
are pulsating.
Recommended
prescription: Atractylodes lancea 15g, Chenpi 10g, Magnolia 10g, Aquilegia 10g,
grass fruit 6g, raw ephedra 6g, Zhihuo 10g, ginger 10g, betel nut 10g.
Suggested use: one dose daily, boiled with 400ml water, take it twice at
morning and evening.
4.2.4 Severe cases 
4.2.4.1 Plague poison and lung-closing
syndrome
Clinical manifestations: fever, flushing, cough, yellowish
phlegm, or blood in sputum, wheezing, shortness of breath, tiredness, fatigue,
dryness and stickiness, nausea, food loss, poor stool, and short urination. Red
tongue, yellow greasy coating, slippery pulses.
Recommended prescription: Raw ephedra 6g, almond 9g, raw
gypsum 15g, licorice 3g, fragrant fragrant 10g (back), Magnolia 10g,
atractylodes 15g, grass fruit 10g, pinellia 9g, Poria 15g, raw rhubarb 5g
(back) 10g, gardenia 10g, red peony 10g.
Suggested use: one or two doses daily, boiled with
100-200ml water, take it 2-4 times, oral or nasal feeding.
4.2.4.2 Syndrome of flaring heat in qifen and yingfen
Clinical manifestations: Hot fever, thirst, shortness of
breath, shortness of breath, blurred vision, or spotted rash, or vomiting
blood, bleeding, or convulsions in the limbs. Tongue ridges have few or no
moss, and the pulse sinks finely, or floats large and counts. Recommended
prescription: 30-60g gypsum (fried first), 30g of Zhimu, 30-60g of raw land,
30g of buffalo horn (fried first), 30g of red sage, 30g of black ginseng, 15g
of forsythia, 15g of paeonia, 6g of peony 12g, gardenia 15g, raw licorice 6g.
Suggested use: 1 dose per day, decoction, first decoct
gypsum and buffalo horn, then apply other pieces, 100ml-200ml each time, 2-4
times a day, orally or nasally.
Recommended Chinese patent medicines: Xiyanping injection,
Xuebijing injection, Reduning injection, Tanreqing injection, Xingnaojing
injection. Drugs with similar efficacy can be selected according to individual
conditions, or can be used in combination according to clinical symptoms.
Traditional Chinese medicine injection can be used in combination with
traditional Chinese medicine decoction.
4.2.5 Critical cases (syndrome of inner
blocking causing collapse)
Clinical manifestations: dyspnea, dyspnea, asthma or need
mechanical ventilation, fainting, irritability, cold sweating, dark purple
tongue, thick or dry moss, large floating roots. Recommended prescription: 15g
of ginseng, 10g of Heishun tablets (decoct first), 15g of dogwood, delivered
with Suhexiang Pill or Angong Niuhuang Pill.
For
patients on mechanical ventilation with abdominal distention or constipation:
5-10g of Dahuang. For patients with human-machine asynchronization: 5-10g of
Dahuang and 510g of Mangxiao while administering sedatives and muscle
relaxants.
Recommended Chinese patent medicines: Xuebijing injection,
Reduning injection, Tanreqing injection, Xingnaojing injection, Shenfu
injection, Shengmai injection, Shenmai injection. Drugs with similar efficacy
can be selected according to individual conditions, or can be used in
combination according to clinical symptoms. Traditional Chinese medicine
injection can be used in combination with traditional Chinese medicine
decoction.
Note: Recommended
usage of Chinese medicine injections for severe and critical cases The use
of traditional Chinese medicine injections follows the principle of
starting from a small dose and gradually adjusting the dosage according to the
instructions of the drug. The recommended usage is as follows:
Viral infection or combined mild bacterial infection: 0.9%
sodium chloride injection 250ml plus Xiyanping injection
100mg bid, or 0.9% sodium chloride injection 250ml heated Duning injection
20ml, or 0.9% sodium chloride injection 250ml plus Tanreqing injection 40ml
bid.
High fever with disturbance of consciousness: 250ml of 0.9%
sodium chloride injection and 20ml bid of Xingnaojing injection.
Systemic inflammatory response syndrome or/and multiple
organ failure: 250ml of 0.9% sodium chloride injection and 100ml of Xuebijing
injection.
Immunosuppression: 250ml of 0.9% sodium chloride injection
and 100ml bid of Shenmai injection.
Shock: 250ml of 0.9% sodium chloride
injection plus 100ml bid of Shenfu injection.
4.2.6 Convalescent period
4.2.6.1 Lung and spleen qi deficiency
syndrome
Clinical manifestations: shortness of breath, fatigue,
fatigue, anorexia, nausea, fullness, weak stool, and uneasiness. The tongue is
pale and greasy.
Recommended prescription: French Pinellia
9g, Chenpi 10g, Codonopsis 15g, Sunburn
Astragalus 30g, Stir-fried Atractylodes
10g, Poria 15g, Huoxiang 10g, Amomum villosum
6g (later), and Licorice 6g
Suggested use: 1 dose per day, boiled with 400ml of water,
twice a day at morning and evening.
4.2.6.2 Qi and Yin deficiency syndrome
Clinical manifestations: Fatigue, shortness of breath, dry
mouth, thirst, palpitations, sweating, poor appetite, low or no lever, dry
cough and little sputum; dry tongue, fine or weak pulses.
Recommended prescription: North and south radix salviae
10g, 15g ophiopogonis, 6g American ginseng, 6g schisandra, 6g gypsum l5g, 10g
light bamboo leaves, 10g mulberry leaves, 15g reed root, 15g salviae
miltiorrhiza, 6g raw liquorice.
Suggested use: 1 dose per day, boiled with 400ml of water,
twice a day at morning and evening.
XI. Discharge criteria and after-discharge
considerations
1.Discharge criteria
1)
Body temperature is back to normal for more than
three days;
2)
Respiratory symptoms improve obviously;
3)
Pulmonary imaging shows obvious absorption of
inflammation,
4)
Nuclei acid tests negative twice consecutively
on respiratory tract samples such as sputum and nasopharyngeal swabs (sampling
interval being at least 24 hours). Those who meet the above criteria can be
discharged.
2.
After-discharge considerations
2.1
The designated hospitals should contact the
primary healthcare facilities where the patients live and share patients’
medical record, to send the information of the discharged patients to the
community committee and primary healthcare facility where the patients reside.
2.2
After discharge, it is recommended for patients
to monitor their own health status in isolation for 14 days, wear a mask, live
in well-ventilated single room if possible, minimize close contact with family
members, separate dinning, practice hand hygiene and avoid going out.
2.3
It is recommended for the patients to return to
the hospitals for follow-up and re-visit in two and four weeks after discharge.
XII. Patients Transportation Principles
Patients should be transported in accordance with the Work Protocol for Transfer of the Novel
Coronavirus Pneumonia Patients (Trial Version) issued by the National
Health Commission.
XIII. Nosocomial Infection Prevention and
Control
Measures
to prevent and control nosocomial infection should be implemented in accordance
with the requirements of the Technical
Guidelines for the Prevention and Control of Infection by the Novel Coronavirus
in Medical Institutions (First Edition) and the Guidelines on the Usage of Common Medical Protective Equipment against
Novel Coronavirus Infection (Trial
Version) formulated by the National Health Commission.
The General Office of National Health
Commission
Office of State TCM Administration
Printed and distributed on March 3, 2020
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