Serpina1 iRNA compositions and methods of use thereof

We claim: 1. A double stranded ribonucleic acid (dsRNA) agent for inhibiting expression of a serine peptidase inhibitor, clade A member 1 (Serpina1) in a cell, wherein said dsRNA agent comprises a sense strand and an antisense strand forming a double-stranded region, wherein the antisense strand comprises at least 19 contiguous nucleotides differing by no more than 3 nucleotides from the nucleotide sequence of 5′-UUUUGUUCAAUCAUUAAGAAGAC-3′ (SEQ ID NO: 419), wherein the sense strand and the antisense strand are each independently 19-25 nucleotides in length, wherein substantially all of the nucleotides of said sense strand and substantially all of the nucleotides of said antisense strand are modified nucleotides, and wherein at least one strand is conjugated to a ligand through a bivalent or trivalent branched linker. 2. The dsRNA agent of claim 1 , wherein one of the 3 nucleotide differences in the nucleotide sequence of the antisense strand is a nucleotide mismatch in the seed region of the antisense strand. 3. The dsRNA agent of claim 1 , wherein the ligand is one or more GalNAc derivatives. 4. The dsRNA agent of claim 1 , wherein said agent further comprises at least one phosphorothioate or methylphosphonate internucleotide linkage. 5. A cell containing the dsRNA agent of claim 1 . 6. A pharmaceutical composition comprising the dsRNA agent of claim 1 . 7. A method of inhibiting Serpina1 expression in a cell, the method comprising (a) contacting the cell with the dsRNA agent of claim 1 , or the pharmaceutical composition of claim 6 ; and (b) maintaining the cell produced in step (a) for a time sufficient to obtain degradation of the mRNA transcript of a Serpina1 gene, thereby inhibiting expression of the Serpina1 gene in the cell. 8. A method of treating a subject having a Serpina1 deficiency variant-associated associated liver disorder, the method comprising administering to the subject a therapeutically effective amount of the dsRNA agent of claim 1 , or the pharmaceutical composition of claim 6 , wherein the subject has one or more of a Serpina1 Z deficiency allele or a Serpina1 PIM(Malton) deficiency allele and the Serpina1 deficiency variant-associated associated liver disorder is associated with the Serpina1 deficiency allele, thereby treating the subject. 9. A method of treating a subject having a Serpina1 deficiency variant-associated liver disorder to reduce the progression of the liver disorder to hepatocellular carcinoma, the method comprising administering to the subject a therapeutically effective amount of the dsRNA agent of claim 1 , or the pharmaceutical composition of claim 6 , wherein the subject has one or more of a Serpina1 Z deficiency allele or a Serpina1 PIM(Malton) deficiency allele and the Serpina1 deficiency variant-associated associated liver disorder is associated with the Serpina1 deficiency allele, thereby treating the subject. 10. A method of reducing the accumulation of misfolded Serpina1 in the liver of a subject having a Serpina1 deficiency variant-associated liver disorder, the method comprising administering to the subject a therapeutically effective amount of the dsRNA agent of claim 1 , or the pharmaceutical composition of claim 6 , wherein the subject has one or more of a Serpina1 Z deficiency allele or a Serpina1 PIM(Malton) deficiency allele and the Serpina1 deficiency variant-associated associated liver disorder is associated with the Serpina1 deficiency allele, thereby reducing the accumulation of misfolded Serpina1 in the liver of the subject. 11. The dsRNA agent of claim 1 , wherein all of the nucleotides of said sense strand and all of the nucleotides of said antisense strand are modified nucleotides. 12. The dsRNA agent of claim 1 , wherein at least one of said modified nucleotides is selected from the group consisting of a 3′-terminal deoxy-thymine (dT) nucleotide, a 2′-O-methyl modified nucleotide, a 2′-fluoro modified nucleotide, a 2′-deoxy-modified nucleotide, a locked nucleotide, an abasic nucleotide, a 2′-amino-modified nucleotide, a 2′-alkyl-modified nucleotide, a morpholino nucleotide, a phosphoramidate, a non-natural base comprising nucleotide, a nucleotide comprising a 5′-phosphorothioate group, and a terminal nucleotide linked to a cholesteryl derivative or a dodecanoic acid bisdecylamide group. 13. The dsRNA agent of claim 1 , wherein at least one strand comprises a 3′ overhang of at least 1 nucleotide; or a 3′ overhang of at least 2 nucleotides. 14. The dsRNA agent of claim 1 , wherein the sense strand is 21 nucleotides in length and the antisense strand is 23 nucleotides in length. 15. The dsRNA agent of claim 3 , wherein the ligand is 16. The dsRNA agent of claim 15 , wherein the at least one ligand is conjugated to the 3′-end of the sense strand. 17. The dsRNA agent of claim 16 , wherein the dsRNA agent is conjugated to the ligand as shown in the following schematic and, wherein X is O or S. 18. The dsRNA agent of claim 17 , wherein the X is 0. 19. The dsRNA agent of claim 1 , wherein the antisense strand comprises the nucleotide sequence 5′-UUUUGUUCAAUCAUUAAGAAGAC-3′ (SEQ ID NO: 419). 20. The dsRNA agent of claim 1 , wherein the sense strand comprises the nucleotide sequence 5′-CUUCUUAAUGAUUGAACAAAA-3′ (SEQ ID NO: 417) and the antisense strand comprises the nucleotide sequence 5′-UUUUGUUCAAUCAUUAAGAAGAC-3′ (SEQ ID NO: 419). 21. The dsRNA agent of claim 1 , wherein the sense strand comprises the nucleotide sequence 5′-csusucuuaauGfAfuugaacaaaa-3′ (SEQ ID NO: 418) and the antisense strand comprises the nucleotide sequence 5′-usUfsuUfgUfuCfaAfucaUfuAfaGfaAfgsasc-3′ (SEQ ID NO: 420), wherein a, g, c, and u are 2′-O-methyl (2′-OMe) A, G, C, and U, respectively; Af, Gf, Cf, and Uf, are 2′-fluoro A, G, C, and U, respectively; and s is a phosphorothioate linkage. 22. The dsRNA agent of claim 21 , further comprising a ligand conjugated to the 3′-end of the sense strand. 23. The dsNA agent of claim 1 , wherein the sense strand consists of the nucleotide sequence 5′-csusucuuaauGfAfuugaacaaaaL96-3′ (SEQ ID NO: 418) and the antisense strand consists of the nucleotide sequence 5′-usUfsuUfgUfuCfaAfucaUfuAfaGfaAfgsasc-3′ (SEQ ID NO: 420), wherein a, g, c, and u are 2′-O-methyl (2′-OMe) A, G, C, and U, respectively; Af, Gf, Cf, and Uf, are 2′-fluoro A, G, C, and U, respectively; s is a phosphorothioate linkage; and L96 is N-[tris(GalNAc-alkyl)-aminododecanoyl)]-4-hydroxyprolinol. 24. A double stranded ribonucleic acid (dsRNA) agent for inhibiting expression of a serine peptidase inhibitor, clade A, member 1 (Serpina1) in a cell, wherein said dsRNA agent comprises a sense strand and an antisense strand forming a double-stranded region, wherein the antisense strand comprises at least 19 contiguous nucleotides differing by no more than 3 nucleotides from the nucleotide sequence of 5′-UUUUGUUCAAUCAUUAAGAAGAC-3′ (SEQ ID NO: 419), wherein the sense strand and the antisense strand are each independently 19-25 nucleotides in length, wherein substantially all of the nucleotides of said sense strand comprise a modification selected from the group consisting of a 2′-O-methyl modification and a 2′-fluoro modification, wherein said sense strand comprises two phosphorothioate internucleoti