Abstract
www.wjpls.org │ Vol 12, Issue 5, 2026. │ ISO 9001:2015 Certified Journal │ 181 UNDER OECD GUIDELINES, ALBINO MICE ANIMAL STUDIES TO STANDARDISE PZ DRUG AGAINST THE REFRACTORY SPIKE PROTEIN INFECTION, HOMO SAPIENS SKIN DEPIGMENTARY DISORDER, CANCER (ALL) A
Dr. S. S. Sawhney*
ABSTRACT
Human system is a bio-automation and self- repairing. The four diseases in reference: spike protein infection,
Homo sapien skin depigmentary disorder, cancer and Hensen problem which have varying root cause, are
exceptional. Complementary characteristics of spike protein, human protein and PZ drug led to the development of
Principles I whereas principles 2, is based upon the epidermal photosensitivity of PZ drug. Principle I fit the bill of
treatment of Homo sapien skin depigmentary disorder, while Principle 2 applies for other diseases. Additionally
Albino mice animal study is equally significant and promising. The cage side observations show no toxicity from
0.5 g and 1 g of drug treatment. The acute toxicity and sub toxicity study show that the body weight of each sex
was significantly (p<0.001) increased in both groups. The organal histopathology (brain, heart, kidney, liver) at 0.5
g and 1.0 g treatment has resulted in normal histopathology status. The biochemistry of Albino mice showed no
significant changes in any of the biochemical parameters when compared with the central group. The above data
and discussion would lead us to the easy and safe, human trials at 0.5 and 1.0 g drug levels and treatments of the
four diseases in reference with PZ drug.
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