生信算法9 - 正则表达式匹配氨基酸序列、核型和字符串
建议在Jupyter实践。
1. 使用正则表达式匹配指定的氨基酸序列
import re# 氨基酸序列
seq = 'VSVLTMFRYAGWLDRLYMLVGTQLAAIIHGVALPLMMLI'# 正则表达式匹配
match = re.search(r'[A|G]W', seq)# 打印match及匹配到开始位置和结束位置
print(match)
# <re.Match object; span=(10, 12), match='GW'>
print(match.start())
print(match.end())if match:# 打印匹配到氨基酸print(match.group())# GW
else:print("no match!")
2. 使用正则表达式查找全部的氨基酸序列
import reseq = 'RQSAMGSNKSKPKDASQRRRSLEPAENVHGAGGGAFPASQRPSKP'# 匹配R开头、第二个氨基酸为任意、第三个氨基酸为S或T、第四个氨基酸不为P的连续4个氨基酸徐磊
matches = re.findall(r'R.[ST][^P]', seq)
print(matches)
# ['RQSA', 'RRSL', 'RPSK']# finditer 匹配对象迭代器
match_iter = re.finditer(r'R.[ST][^P]', seq)# 遍历
for match in match_iter:# 打印group和spanprint(match.group(), match.span())print(match.start(), match.end())# RQSA (0, 4)# 0 4# RRSL (18, 22)# 18 22# RPSK (40, 44)# 40 443. 使用正则表达式匹配多个特殊字符,分割字符串
import re# 匹配特殊字符|和;,并分割字符串
annotation = 'ATOM:CA|RES:ALA|CHAIN:B;NUMRES:166'
split_string = re.split(r'[|;]', annotation)print(split_string)
# ['ATOM:CA', 'RES:ALA', 'CHAIN:B', 'NUMRES:166']4. 正则表达式获取核型染色体数量,区带和CNV大小
karyotype1 = '46,XY; -11{p11.2-p13, 48.32Mb}'
karyotype2 = '47,XXX; +X{+3};-11{p11.2-p13.2, 48.32Mb}'#### 匹配染色体数量 ####
match = re.search(r'(\d+,\w+);', karyotype1)
print(match)
# <re.Match object; span=(0, 6), match='46,XY;'>chr = match.group(1)
print(chr)
# 46,XY#### 匹配染色体开始和结束区带和CNV大小 ####
match2 = re.search(r'([p|q|pter]\d+.?\d+)-([p|q|qter]\d+.?\d+), (\d+.?\d+)Mb', karyotype2)
print(match2)cyto_start = match2.group(1)
cyto_end = match2.group(2)
size = match2.group(3)print(cyto_start)
# p11.2
print(cyto_end)
# p13.2
print(size)
# 48.32
5. 正则表达式获取指定格式的字符串内容
# 结果变异VCF文件描述信息
string = """##ALT=<ID=DEL,Description="Deletion">##ALT=<ID=DUP,Description="Duplication">##ALT=<ID=INV,Description="Inversion">##ALT=<ID=INVDUP,Description="InvertedDUP with unknown boundaries">##ALT=<ID=TRA,Description="Translocation">##ALT=<ID=INS,Description="Insertion">##FILTER=<ID=UNRESOLVED,Description="An insertion that is longer than the read and thus we cannot predict the full size.">##INFO=<ID=CHR2,Number=1,Type=String,Description="Chromosome for END coordinate in case of a translocation">##INFO=<ID=END,Number=1,Type=Integer,Description="End position of the structural variant">##INFO=<ID=MAPQ,Number=1,Type=Integer,Description="Median mapping quality of paired-ends">##INFO=<ID=RE,Number=1,Type=Integer,Description="read support">##INFO=<ID=IMPRECISE,Number=0,Type=Flag,Description="Imprecise structural variation">##INFO=<ID=PRECISE,Number=0,Type=Flag,Description="Precise structural variation">##INFO=<ID=SVLEN,Number=1,Type=Integer,Description="Length of the SV">##INFO=<ID=SVMETHOD,Number=1,Type=String,Description="Type of approach used to detect SV">##INFO=<ID=SVTYPE,Number=1,Type=String,Description="Type of structural variant">##INFO=<ID=SEQ,Number=1,Type=String,Description="Extracted sequence from the best representative read.">##INFO=<ID=STRANDS2,Number=4,Type=Integer,Description="alt reads first + ,alt reads first -,alt reads second + ,alt reads second -.">##INFO=<ID=REF_strand,Number=.,Type=Integer,Description="plus strand ref, minus strand ref.">##INFO=<ID=Strandbias_pval,Number=A,Type=Float,Description="P-value for fisher exact test for strand bias.">##INFO=<ID=STD_quant_start,Number=A,Type=Float,Description="STD of the start breakpoints across the reads.">##INFO=<ID=STD_quant_stop,Number=A,Type=Float,Description="STD of the stop breakpoints across the reads.">##INFO=<ID=Kurtosis_quant_start,Number=A,Type=Float,Description="Kurtosis value of the start breakpoints across the reads.">##INFO=<ID=Kurtosis_quant_stop,Number=A,Type=Float,Description="Kurtosis value of the stop breakpoints across the reads.">##INFO=<ID=SUPTYPE,Number=.,Type=String,Description="Type by which the variant is supported.(SR,AL,NR)">##INFO=<ID=STRANDS,Number=A,Type=String,Description="Strand orientation of the adjacency in BEDPE format (DEL:+-, DUP:-+, INV:++/--)">##INFO=<ID=AF,Number=A,Type=Float,Description="Allele Frequency.">##INFO=<ID=ZMW,Number=A,Type=Integer,Description="Number of ZMWs (Pacbio) supporting SV.">##FORMAT=<ID=GT,Number=1,Type=String,Description="Genotype">##FORMAT=<ID=DR,Number=1,Type=Integer,Description="# high-quality reference reads">##FORMAT=<ID=DV,Number=1,Type=Integer,Description="# high-quality variant reads">"""import re# 创建空dataframe
df_output = pd.DataFrame()list_type = []
list_id = []
list_description = []# 遍历字符串内容,内容拷贝至结构变异VCF文件
for str in string.split('\n'):# 去除末尾\n和字符串内空格str = str.strip().replace(' ', '')# 内容为空或字符串为空则跳过if not str or str == '':continue# 正则表达式匹配##后的英文字符match = re.search(r'##(\w+)', str)type = match.group(1) if match else 'ERORR'# 匹配ID内容match = re.search(r'ID=(\w+)', str)id = match.group(1) if match else 'ERORR'# 匹配Description内容match = re.search(r'Description=\"(.*?)\"', str)description = match.group(1) if match else 'ERORR'# 加入列表list_type.append(type)list_id.append(id)list_description.append(description)print(list_description)
# 加入dataframe
df_output['Type'] = list_type
df_output['ID'] = list_id
df_output['Description'] = list_description# 保存至excel
df_output.to_excel('结构变异描述信息说明.xlsx', index=False)
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