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Rubiaccae
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Herb
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Emetic
root
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The
Od Force of the root of the plant is used as one of the components in the
preparation of the remedy.
The
material or chemical strong expectoration function takes place at the cost of
happening of severe vomiting and diarrhea as the chemical reaction of the
material with human chemical is caused to make the suffering human system more
deficient in the fund of the constructional energy (Od Force) in expectorating function
with the corresponding loss of the matter of the cells. This incidence speaks
of the matter that the cell to cell negatively charged electromagnetic
circuit(s) concerning the lungs’ expectoration here is unexpectedly linked with
the cell to cell negatively charged electromagnetic circuit(s) concerning the
severe vomiting and diarrhoea. So it lifts the induced vomiting.
It exhibits the inhibition of
the protein synthesis. It withdraws the diversions or shifts caused from the
infestation of protozoa the human system and chemical reactions between the human
system’s cells and protozoa. It is anti-amoebiasis. Material or chemical
activities punishing the protozoa and amoebiasis causes muscular contraction
leading to cardiac failure are washed of herewith. It withdraws in this way the
risk of developing or developed proximal myopathy and/or cadiomyopathy. Material or chemical interference with muscle
contractions leading to cardiac failure is
withdrawn herewith. It
withdraws the chemical or material shifts or diversions caused by
fascioloidiasis.
In fact it is highly capable of erasing the
chemical diversions or shifts caused by viral, parasitic organisms,
anti-cancer, and contraceptive chemical reactions based activities. It exhibits
the inhibition of both ribosomal and mitochondrial protein synthesis and interferes with the synthesis and activities of
DNA and RNA. Caused up-regulation and down-regulation of a number of genes are
reversed herewith.
It exhibits the
inhibition of the aminoacyl-sRNA transfer reaction by reversing all the series
of steps that result to incorporate the aminoacyl moiety into polypeptide-bond
form. This Od Force breaks the chemical irreversibility to exhibits the
inhibited protein synthesis in HeLa cells by augmenting the depleted number of
free ribosomes and subsequently decreasing the increased the polyribosomes. It
withdraws the chemical or material diversions of shifts in the process of
inhibition of viral RNA synthesis in poliovirus-infected HeLa cells. This
exhibition of the RNA inhibition progressing from being reversible to
irreversible is broken herewith. Prevention of induced autophagy in exocrine
cells of pancreas and seminal vesicle by stabilizing polyribosomes occurs with
accompaniment of inhibiting protein synthesis. The caused chemical or material
diversions or shifts to give the effect of prevention are cancelled herewith.
The chemistry that blocks the early S phase of DNA replication is rewind here
again. The chemistry of reducing DNA, RNA and protein synthesis of thymic cells
is also cancelled herewith.
The caused diversion and shifts from the material or
chemical treatment of amoebic liver and perianal skin amoebiases, both of which
are caused by the same parasite are withdrawn herewith. Thus the new focus of the expression of the
addition of the further loss of the Od Force with previous loss of the Od Force
caused in the process of infestation and gross chemical entry in the requisite
sites due to the toxicity or excessive toxicity is reversed herewith. Reduction
of cytoplasmic volume, maintenance of plasma cell integrity, and production of
nuclear condensation and DNA fragmentation caused chemically or by the
infestation is hereby withdrawn. The Od Force in question is potent enough in
antileishmanial activity against Leishmania donavani. It is equally smart in
tackling as the trypanocidal agent against Trypanosoma cruzi against Chaga’s
disease. It displays trypanocidal activity against Trypanosoma brucei also.
Evaded
immune response by continuous antigenic variation on the surface coat of the
human cell, caused loss of various B cell populations, disability to raise a long-lasting specific protective
anti-parasite antibody response, abrogated vaccine-induced protective response are
redirected herewith. Remodeling of spleen and the rapid loss of the IgM+ marginal zone (IgM+MZ) B cell
population are reversed herewith. Increased caspase-3 enzyme activity and
elevated caspase-3 mRNA levels coincided with decreased mRNA levels of the
anti-apoptotic Bcl-2 protein and BAFF receptor (BAFF-R), indicating the onset
of apoptosis, are rewind herewith. The affected B cells became unresponsive to
stimulation by BCR cross-linking with anti-IgM Fab fragments is become
herewith. Infection-induced loss of IgM+ B cells coincided with the disappearance of
protective variant-specific T-independent IgM responses, rendering the host
rapidly susceptible are withdrawn herewith. Infections with T. brucei parasites result in the rapid loss of
T–cell independent IgM+MZ B cells that are normally functioning as
the primary immune barrier against blood-borne pathogens are established herewith.
It is antipoxviral. It shows significant antiviral activity
against dengue virus. The chemical or material shifts from the causation of the
inhibition of vaccinia virus replication are also erasable herewith. It washes
the chemical or material diversion caused from the treatment of murine L-1210 and P-388 leukemia, caused apoptotic
cytotoxicity in many human cancer cell lines: U937 (leukaemic cell line),
A549-S (lung adenocarcinoma), Jurkat T cells (T cell leukemia), CCRFCEM (Human
T cell lymphoblast-like cell line), HL-60 (Human promyelocytic leukemia cells)
and CEM/ADR5000 (leukemia cell line). The inhibition of protein synthesis and
interaction with DNA causing cytotoxicity are reversed herewith. Not only the protein synthesis inhibition and
interaction with DNA induced apoptosis by regulation of pro-apoptotic factors
is also rewind. Regulation on alternative splicing of Bcl-x pre-mRNA by protein
phosphatase I is also reversed.
Down-regulated levels of the antiapoptotic variant Bcl-xL mRNA, and
up-regulated levels of the pro-apoptotic variant Bcl-xS mRNA undergo reversion
also. The material or chemical diversion from the decrease of the Bcl-xL/Bcl-xS
ratio in MCF-7 breast cancer, PC3-prostate cancer, C33A-cervical cancer and
A549-lung cancer cell lines enjoy an anti-truck passage in the good of this Od
Force. The up-regulation of some pro-apoptotic and anti-survival genes: BAK1,
CASP8 (caspase 8), CASP9 (caspase 9), DAXX (death-associated protein 6), GZMB
(granzyme B) and TNFRSF6 into Jurkat cells after treatment is cancelled
herewith. BCL2, EGFR (epidermal growth factor receptor), and TNF (tumor
necrosis factor), are anti-apoptotic and prosurvival genes in Jurkat cells
and downregulation of these is similarly
cancelled herewith. The anti-apoptotic and pro-survival genes (AKT1, MST1,
TNFRSF11B, and TNFSF13) as are upregulated in Jurkat cells are also reversed.
The chemical or material diversions from caused phosphatidylserine exposure,
mitochondrial depolarization, and DNA fragmentation in Jurkat T-cells are also
made travelled in the path along which it came once. Apart from genes that are
directly linked to apoptosis, this Od Force is also capable of withdrawing the
affect of the expression of other genes. The matrix metalloproteinase (MMP)
gene family includes 24 genes involved in tissue remodeling and their dysregulation
is observed in many pathological conditions, including cancer. Blocked induction of all genes except MMP9
and TIMP3 is also withdrawing herewith. Increasing PGC-1 activity controlling
muscular dystrophy, diabetes, neurodegenerative diseases and ovarian cancer is
withdrawn herewith. Increasing PGC-1 activity in the ovarian cancer cell line
Ho-8910 inducing apoptosis is withdrawn herewith simultaneously.
The uterus and early
embryos around implantation, possibly the trophoblast and endometrial cells at
the attachment site is the main target of the action of this Od Force to lift
the early implantation hazards.
The loss of the Od
Force due to nonsense-mediated decay (NMD), the mechanisms cells used to
prevent the synthesis of truncated protein (gene expression) or mutant genes
that lead to human diseases is meet up herewith. Inhibition of NMD stabilizes
the mutant transcripts and identifies the genes containing the truncated mutant.
The material or chemical shifts or deviation from this protein synthesis
inhibition of NMD combined with microarrays influences the prostate cancer cell
lines (DU145, PC3, and LnCaP) to reverse the mutations of EPHB2 in human
prostate cancer, mutations in colon cancer cells and melanoma.
It withdraws the toxicity
of myopathy, in addition, cardiotoxicity, including cardiomyopathy. It lifts the activity of the adrenergic (2)
blocker and exhibits inhibitor of dipeptidyl aminopeptidase IV. It similarly
cancels the activity of the antagonist of dopamine (D1 and D3) receptors, substance
P, and neurokinin NK3 to establish the previous state.
It exhibits the inhibited
ribosomal and mitochondrial protein synthesis and interferes with the synthesis
and activities of DNA and RNA. It is used as an
amebicide to instant repair of the damages done due to amoebiasis and cause
withdrawal of serious cardiac, hepatic, or renal damage and violent diarrhea
and vomiting by removal of the loss of the Od Force concerned with the instant
supply of the same. It exhibits the inhibited protein synthesis in eukaryotic
cell, not in prokaryotic cells. It is done by unbinding the material or
chemical binding done to the 40S subunit of the ribosome. Mutants resistance altered
in the 40S ribosomal subunit (S14 protein) is rewind herewith. The exhibited
cross-resistance is withdrawn but not other inhibitors of protein synthesis. The compounds to which these mutants
exhibit cross-resistance suffer the change in chemistry to register this
exhibition.
Irritation of the cutaneous and mucous
surfaces is removed herewith. Not only that the material or chemical activity
that excites irritation, and produces vesicular, pustular and sometimes
ulcerative effects in the skin is also withdrawn. Exceeding irritation to the
Schneiderian membrane, causing heat and violent sneezing is also under the
coverage of the activity of this Od Force. Provoked decided paroxysms, closely
resembling spasmodic asthmatic attacks—the chief symptoms being great dyspnoea,
with marked anxiety and prostration, and wheezing respiration and cough,
bronchitis with croup are also subjects of this Od Force. This is often
accompanied with violent and prolonged sneezing and spitting of blood, usually
followed by free expectorating mucus are also erased herewith. The new focus of
the loss of Od Force from material or chemical activity may be expressed as to
cause gastric tonicity and hepatic stimulation is also withdrawn. Produced
emesis and hence catharsis as usually results is also cancelled herewith. The
relaxation of the skin and consequent diaphoresis and increased the
broncho-pulmonic secretions are withdrawn herewith. Including the Physiological
scarce effect in the circulation the stimulation over the circulatory apparatus
are lifted herewith. Therapeutic action upon the circulation giving effects
upon hemorrhage; and in acute disorders of the stomach, bowels, and breathing organs are also in
the range of its target.
This Od Force is a very important to lift the provocation
over emesis, to check active hemorrhages, to relieve gastro-intestinal and
broncho-pulmonic irritation and inflammations, cardiac paralysis. It is best
observed in the material or chemical shifts or deviation caused from acute
affections, when there is hyperemia, capillary engorgements, and
hyper-secretion.
Material or chemical
actions in active hemorrhages—post-partum, hemoptysis, hematemesis, hematuria, epistaxis, and hemorrhages from the bowels
opens a new focus to balance the addition of further deficiency of the Od Force
from their previous focus at capillary. The nervousness with marked
irritability and vascular excitation suffers the additive loss of the Od Force
in some new focus. The chemical or material diversion or shift from menorrhagia and metrorrhagia, hemorrhoids, especially when of the
bleeding variety are also rewind herewith.
It is very efficient in withdrawing the chemical or material
deviation or shift from the night-sweats of consumption, the majority of cases of phlyctenular diseases of
the eye with photophobia. It is also extremely valuable in erasing the
chemical or material diversion or shift from peritonitis, even the worst form occurring in puerperal women. It is also
of value in withdrawing the focuses of acute rheumatism, gout,
jaundice from materially or chemically
treated biliary catarrh, and to heal the relaxed parts in the passage of
small biliary calculi.
Materially or chemically caused nausea, vomiting, stomach
irritation, dizziness, low blood pressure, shortness of breath, fresh
heartburn, irritation of skin and respiratory tract, serious poisoning including
difficulty breathing, digestive tract problems, uncontrolled heart rates, bleeding in urine,
convulsions, shock, coma, and death are withdrawn herewith.
Stimulated uterus causing miscarriage is also rewinding. In breast feeding it is safe. It is
also capable to cancel serious complications including damage of the esophagus including ulcers, infection or Crohn’s disease, pneumonia. It is
anti-diaphoretic. Costing of improved appetite materially or chemically is
cancelled herewith to give back the human system that was suffering from
anorexia. The deviations or shifts from the intravenous material or chemical
uses for hepatitis and pockets of infection (abscesses) are cancelled herewith
to rewind the staged chemical process. Chemical or material activities that
irritate the digestive tract and trigger the brain to cause vomiting are withdrawn herewith.
The
material or chemical irritant effect on the
gastrointestinal tract or mucosal erosions of the entire gastrointestinal tract
generally induces to persistent bloody vomiting or diarrhea but those effects
may give rise to adverse effects on the heart, such as conduction abnormalities
or myocardial infarction. These, in combination with dehydration, may cause
vasomotor collapse followed by death. Induced
vomiting in eating disorders has been implicated in the diagnosis of cardiotoxicity
and myopathy. All these are rewinding or reversed herewith. Adverse effects of
repeated vomiting, such as metabolic complications, aspiration pneumonitis,
parotid enlargement, dental abnormalities, and oesophagitis or haematemesis due
to mucosal lacerations Cardiovascular
toxicity, manifesting as muscle weakness, hypotension, palpitations and arrhythmias
are the victims of this Od Force The load of chemistry leading to gastric
rupture, Mallory-Weiss lesions of the oesophagogastric junction, cerebrovascular
events, pneumomediastinum and pneumoperitoneum, allergy characterized by
rhinitis, conjunctivitis and chest tightness are also the subjects of it.
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