KR0178422B1 - Liposome comprising hantan virus derived peptide antigen - Google Patents

Abstract

The present invention relates to liposomes sensitive to pH containing peptide antigens derived from the N, G1 and G2 proteins of Hantan virus. Since the liposomes of the present invention can cause cellular immunity, which induces the production of cytotoxic T lymphocytes specific for the electric virus, it can be used for the prevention and treatment of the disease of Hantan virus. .

Description

Liposomes Containing Peptide Antigens of Hantan Virus

The present invention relates to liposomes containing the peptide antigens of hantan virus. More specifically, the present invention provides a liposome formulation of peptide antigens derived from the N, G1 and G2 proteins of the Hantan virus to induce the production of cytotoxic T lymphocytes ('CTL') specific for the electric virus. It relates to liposomes that cause cellular immunity.

Viral diseases have constantly plagued humans, but no groundbreaking cure has been found to this day. However, only the protection by preventive vaccines is possible, but in the case of the Hantan virus (Hantaan virus) in which the preventive vaccine has been developed, the infected patients continue to occur, and the drug that can provide the fundamental treatment for the viral disease that occurred once It is not developed.

Cellular immunity is achieved by several types of cells belonging to the lymphatic system, which have the ability to directly destroy cells and tissues infected by bacteria or viruses. Therefore, cellular immunity exerts its function effectively, such as intracellular infection of bacteria or viruses, or cancer cells.

Therefore, in the present invention, the peptide fragrance originated from the Hantan virus was formulated to induce CTL production of the peptide antigen by formulating liposomes.

In general, when phospholipids are dispersed in water, the hydrophobic head of the phospholipid is directed towards the water, and the hydrophobic tails are combined by hydrophobic interactions between the tails. It forms a spherical closed endoplasmic reticulum of a bilayer, which is called a 'liposome'. These liposomes have not only been used as models of biofilms, but also widely used as delivery media for drugs (Lee, JW and Kim, H., Arch. Biochem. Biophys., 297: 354 (1992); Hahn). , KH and Kim, H., J. Biochem., 110: 635 (1991); Yun, CH and Kim, H., J. Biochem., 105: 406 (1989); Kim, J. and Kim, H. , Biochemistry, 25: 7867 (1986); Kim, J. and Kim, H., Korean Biochem. J., 18: 403 (1985)).

Recently, liposomes have also been used in the field of immunology, and the use of liposomes as carriers or adjuvants of vaccines has been intensively studied (Rooijen, N.V., Vaccine, 11: 1170 (1993)). In general, intravenous injection of liposomes is easily captured by macrophage ('Mo') which is present in large amounts in the blood. MO is not only important for the immunological processing of antigens, but also plays a very important role in the processing of liposome antigens.

In addition, methods of inducing selective CTL production in viruses using recent pH-sensitive liposomes (Readdy, R. et al., J. Immunol. Methods. 141: 157 (1991); Zhou, F. et al., J. Immunol.Methods, 145: 143 (1991); Nair, S. et al., J. Exp. Med., 175: 609 (1992); Harding, CV et al., 147: 2860 (1991); Zhou, F. and Huang, L., Vaccine, 11: 1139 (1993)) have been widely used as carriers or immunoadjuvant for therapeutic vaccines. Accordingly, the present inventors also applied for a method for preparing a pH-sensitive liposome capable of selective delivery of an anticancer drug (Choi, MJ et al., J. Biochem., 112: 694 (1992)) and its composition. (Reference: Korean Patent Application Nos. 93-18389 and 93-18390).

The inventors of the present invention prepare a liposome with a phospholipid composition of a pH-sensitive liposome, which has been patented and known as described above, and captures a peptide antigen recognized by CTL among the N, G1 and G2 proteins of the Hantan virus, To prepare a liposome containing peptides that can induce specific cellular immunity, the present invention has been completed for the purpose of using them for the prevention and treatment of diseases of the hantan virus.

After all, it is an object of the present invention to provide a liposome comprising a peptide antigen derived from a hantan virus and inducing cellular immunity.

Amino acid sequences used in the present invention are abbreviated as follows according to the IUPAC-IUB nomenclature:

Hereinafter, the present invention will be described in more detail.

Phosphatidylethanolamine-β-oleoyl-r-palmitoyl: POPE and Cholesterol Hemisuccinate to Prepare pH-Sensitive Liposomes Containing Peptide Antigens Derived from Hantan Virus (ch olesterol hemisucci nate: CHOH) in a molar ratio of 6: 4 to 8: 2, most preferably 7: 3, or POPE / PE (phosphatidylethanolamine) / CHOH in a molar ratio of 3: 3: 4 to 4: 4 : 2, most preferably 3.5: 3.5: 3, so that the phospholipids formed form a thin film, which is then recognized by CTL among the peptide antigens derived from the peat virus, ie the N, G1 and G2 proteins of the peat virus A buffer in which the peptide antigen was lysed was added. At this time, the liposome containing a peptide antigen derived from a hantan virus is prepared by mixing one or more peptide antigens and phospholipids in a molar ratio of 1: 5 to 1:25, most preferably 1:20. In addition, the pH-sensitive liposomes prepared by the present invention may further comprise 1 mol% monophosphoryl lipid A as phospholipids.

In the present invention, the peptide antigen derived from the Hantan virus is added to 1 to 5 amino acids before and after the electric peptide, as well as a peptide including the 9 amino acids shown in Table 1 of Example 1, which will be described later, according to the spirit of the present invention. And all peptides and functional equivalents thereof. In the present invention, the term "functional equivalent" means all peptides in which one or two of the amino acid sequences of the peptide are substituted. For example, substitutions may include Gly, Ala; Val, Ile, Leu; Asp, Glu; Asn, Gln; Ser, Thr; Lys, Arg; And combinations such as Phe, Tyr.

The former peptide-containing liposomes capture peptide antigens that can induce CTL production in humans among the N, G1 and G2 proteins of Hantan virus, and pH-sensitive liposomes, which are carriers of peptides, are also the source of the peptides. Since it is known to induce CTL production specific to viruses (see Korean Patent Application No. 94-22792), it will induce cellular immunity in humans.

Hereinafter, the present invention will be described in more detail with reference to Examples. These examples are only for illustrating the present invention, and it will be apparent to those skilled in the art that the scope of the present invention is not limited to these examples.

Example 1

[Preparation of pH Sensitive Liposomes Containing Peptide Antigen]

Phospholipids with POPE / CHOH (7: 3 molar ratio) or phospholipids with POPE / PE / CHOH (3.5: 3.5: 3 molar ratio) are placed in glass vials and dissolved in an organic solvent. Blown in to form a thin film in the vial. Then, hydrated sufficiently by adding a buffer solution (pH 8.0) in which the peptide to be captured was dissolved and vigorously stirred to prepare a superimposed multilamellar vesicle (MLV), and using an ultrasonic sonicator. Small unilamellar vesicle (SUV) was prepared. The SUV thus prepared was left at room temperature for 2 to 12 hours, then rapidly frozen with liquid nitrogen and then thawed slowly at room temperature for 3 to 4 times to prepare a liposome containing peptides. The liposomes containing the peptide thus prepared are prepared by mixing the peptide and the phospholipid at a molar ratio of 1:20, and the peptides used are as shown in Table 1 below. Peptides with functions. At this time, the peptide not contained in the liposome was removed by passing through a Sephadex G-50 column (1 × 20 cm) to obtain only the liposome solution.

The peptide-containing liposomes thus obtained were found to have excellent physical stability due to less destruction by ethanol, and the degree of leakage of liposome contents was much less than that of conventional pH-sensitive liposomes (see Korean Patent Application No. 93-18390). .

As a result, the peptide captured in the peptide-containing liposome prepared above is a peptide antigen that induces CTL production among the N, G1 and G2 proteins of the Hantan virus, and the origin of the peptide captured in the pH-sensitive liposome, which is a carrier of the peptide From reports of inducing CTLs specific for specific viruses (see Korean Patent Application No. 94-22792), the natural results suggest that the peptide-containing liposomes of the present invention will cause cellular immunity that induces CTL production in humans. do.

As described and demonstrated in detail above, the present invention provides a peptide-sensitive liposome that contains a peptide antigen derived from the Hantan virus and is capable of inducing cellular immunity against the Hantan virus. Therefore, these liposomes can be used for the prevention and treatment of Hantan virus-related diseases.

Claims (2)

(i) phosphatidylethanolamine-β-oleyl- -palmitoyl and cholesterol hemisuccinate in a molar ratio of 6: 4 to 8: 2 Phospholipids mixed with; And (ii) a peptide antigen derived from a hantan virus comprising the following amino acid sequence such that the content of the peptide antigen that induces the production of cytotoxic T lymphocytes with respect to the electrophospholipid is from 5: 1 to 25: 1 molar ratio. PH sensitive liposomes containing at least one of: SMLSYGNVL YLTSFVVPI ILLKALYML GLYPAQIKA KLLPDTAAV TLAQSLIDV VMASLVWPV GIFSGNWIV VLLSILCPV In the above, amino acid sequences are described according to the nomenclature of IUPAC-IUB. The pH-sensitive liposome according to claim 1, wherein the phospholipid further comprises 1 mol% monophosphoryl lipid A.